Analogy of ribosome
Hogwarts, but unexpected instead
2015.08.05 17:02 Moose_Hole Hogwarts, but unexpected instead
Hogwarts, unexpectedly This sub is a meta-sub documenting the instances where the World of Harry Potter comes up as an analogy, joke or metaphor on online discussions.
2009.09.27 06:05 cinsere Quantum Mechanics - Physics Community
Scientific discourse about quantum mechanics and related fields. Not for discussions about interpretations or speculative theories.
2012.11.12 05:01 DecRand Bad Analogies: As dead as an alive thing
/badanalogies. A place to post all those bad analogies, metaphors and similes found throughout your travels on the internet.
2024.04.06 19:10 cats64sonic Divine Code: Exploring Christianity and the Mysteries of DNA Transcription and Translation
Introduction:
Christianity, one of the world's major religions, has left an indelible mark on human history, shaping cultures, societies, and moral values for over two millennia. Amidst its theological teachings and spiritual insights, the study of DNA transcription and translation offers a fascinating lens through which to explore the intricate mechanisms of life and the divine order believed by many Christians to underpin creation. This essay delves into the intersection of Christianity and DNA transcription and translation, uncovering parallels between theological concepts and molecular biology.
Christianity's Concept of Creation and Order:
At the heart of Christian theology lies the belief in a divine creator who fashioned the universe and all living beings according to a grand design. The Book of Genesis in the Christian Bible recounts the story of creation, portraying God as the master architect who brought order out of chaos and breathed life into the world. This narrative underscores the divine purpose and inherent harmony believed to pervade all aspects of creation, from the vast cosmos to the microscopic realm of molecular biology.
DNA: The Blueprint of Life:
DNA (deoxyribonucleic acid) serves as the blueprint of life, encoding the genetic instructions necessary for the development, growth, and functioning of all living organisms. Within the double helix structure of DNA lies the code that dictates the sequence of amino acids in proteins, the building blocks of cells and tissues. The intricate arrangement of nucleotide base pairs in DNA determines the unique characteristics and traits of each individual, reflecting the divine craftsmanship believed by Christians to be inherent in creation.
Transcription: The Word Made Flesh:
DNA transcription is the process by which the genetic information encoded in DNA is transcribed into messenger RNA (mRNA), a single-stranded molecule that carries the genetic code from the nucleus to the cytoplasm of the cell. In a metaphorical sense, DNA transcription can be likened to the act of divine revelation, where the hidden mysteries of the genetic code are made manifest in the material world. Just as the Word of God was made flesh in the person of Jesus Christ, DNA transcription brings forth the manifestation of genetic information into tangible form, guiding the development and functioning of living organisms.
Translation: The Language of Life:
DNA translation is the process by which the genetic code carried by mRNA is translated into the sequence of amino acids that make up proteins. This process occurs within the ribosomes, complex molecular machines that serve as the cellular factories for protein synthesis. In Christian theology, translation can be seen as analogous to the incarnation of Christ, where the divine Word is made
incarnate in human form. Just as Jesus Christ serves as the mediator between God and humanity, proteins act as the mediators between the genetic code and the diverse functions of living organisms, facilitating cellular processes and maintaining the integrity of life.
Divine Harmony and Molecular Biology:
The study of DNA transcription and translation offers insights into the profound interconnectedness between theology and molecular biology, highlighting the parallels between Christian beliefs and the mechanisms of life. The intricate processes of genetic expression and protein synthesis reflect the divine order believed by Christians to permeate all aspects of creation, from the macroscopic to the microscopic. By unraveling the mysteries of DNA transcription and translation, we gain a deeper appreciation for the intricate design and purpose that underlie the complexity of life on Earth.
Conclusion:
Christianity and DNA transcription and translation intersect in profound ways, illuminating the divine order and purpose believed by many Christians to underpin the fabric of creation. Through metaphorical parallels between theological concepts and molecular processes, we gain insights into the interconnectedness of faith and science, spirituality and biology. As we continue to explore the mysteries of DNA and unravel the secrets of life, we honor the theological traditions that inspire wonder and reverence for the divine craftsmanship manifested in the natural world.
submitted by cats64sonic to DecreasinglyVerbose [link] [comments]
Christianity, one of the world's major religions, has left an indelible mark on human history, shaping cultures, societies, and moral values for over two millennia. Amidst its theological teachings and spiritual insights, the study of DNA transcription and translation offers a fascinating lens through which to explore the intricate mechanisms of life and the divine order believed by many Christians to underpin creation. This essay delves into the intersection of Christianity and DNA transcription and translation, uncovering parallels between theological concepts and molecular biology.
Christianity's Concept of Creation and Order:
At the heart of Christian theology lies the belief in a divine creator who fashioned the universe and all living beings according to a grand design. The Book of Genesis in the Christian Bible recounts the story of creation, portraying God as the master architect who brought order out of chaos and breathed life into the world. This narrative underscores the divine purpose and inherent harmony believed to pervade all aspects of creation, from the vast cosmos to the microscopic realm of molecular biology.
DNA: The Blueprint of Life:
DNA (deoxyribonucleic acid) serves as the blueprint of life, encoding the genetic instructions necessary for the development, growth, and functioning of all living organisms. Within the double helix structure of DNA lies the code that dictates the sequence of amino acids in proteins, the building blocks of cells and tissues. The intricate arrangement of nucleotide base pairs in DNA determines the unique characteristics and traits of each individual, reflecting the divine craftsmanship believed by Christians to be inherent in creation.
Transcription: The Word Made Flesh:
DNA transcription is the process by which the genetic information encoded in DNA is transcribed into messenger RNA (mRNA), a single-stranded molecule that carries the genetic code from the nucleus to the cytoplasm of the cell. In a metaphorical sense, DNA transcription can be likened to the act of divine revelation, where the hidden mysteries of the genetic code are made manifest in the material world. Just as the Word of God was made flesh in the person of Jesus Christ, DNA transcription brings forth the manifestation of genetic information into tangible form, guiding the development and functioning of living organisms.
Translation: The Language of Life:
DNA translation is the process by which the genetic code carried by mRNA is translated into the sequence of amino acids that make up proteins. This process occurs within the ribosomes, complex molecular machines that serve as the cellular factories for protein synthesis. In Christian theology, translation can be seen as analogous to the incarnation of Christ, where the divine Word is made
incarnate in human form. Just as Jesus Christ serves as the mediator between God and humanity, proteins act as the mediators between the genetic code and the diverse functions of living organisms, facilitating cellular processes and maintaining the integrity of life.
Divine Harmony and Molecular Biology:
The study of DNA transcription and translation offers insights into the profound interconnectedness between theology and molecular biology, highlighting the parallels between Christian beliefs and the mechanisms of life. The intricate processes of genetic expression and protein synthesis reflect the divine order believed by Christians to permeate all aspects of creation, from the macroscopic to the microscopic. By unraveling the mysteries of DNA transcription and translation, we gain a deeper appreciation for the intricate design and purpose that underlie the complexity of life on Earth.
Conclusion:
Christianity and DNA transcription and translation intersect in profound ways, illuminating the divine order and purpose believed by many Christians to underpin the fabric of creation. Through metaphorical parallels between theological concepts and molecular processes, we gain insights into the interconnectedness of faith and science, spirituality and biology. As we continue to explore the mysteries of DNA and unravel the secrets of life, we honor the theological traditions that inspire wonder and reverence for the divine craftsmanship manifested in the natural world.
2024.03.29 03:05 Rthadcarr1956 The Compatibilist Dichotomy
Compatibilism is the philosophical position that people have free will even if determinism is in fact true. Determinism is the premise that all present and future actions are completely entailed by the past along with the laws of nature. So determinism holds that what you are thinking about right now is a direct and inescapable result of the state of the universe before the Earth was formed. All of your actions are completely predetermined and you have no ability to alter the future that the laws of nature prescribe. Indeed, you are just part of the inexorable playing out of reality that was set in motion billions of years ago (by some magic that determinists don’t talk about). So the dichotomy is: how can you reconcile this deterministic viewpoint with a belief that an individual has agency and the ability to make free will choices?
I analogize compatibilism to building a bridge starting on the opposite banks of a river. It is easy to get started on either side, but the real trick is to get them to meet in the middle. So on one bank of the river you have this deterministic view where classical physics is obviously deterministic and on the opposite shore you have free willed actions of the individual. The trick is to connect the two while not contradicting either one. Let’s begin with the idea of free will. Free will is the default position that most everyone operates under. Free will means that in many situations we have a limited freedom to choose between different options. We can decide when to turn right or go straight, when to go to work and when to stay home, and the whole panoply of choices we make every day. We often reflect on the important choices we make and evaluate how good of a choice we made. Not that we can go back and change things, but we can learn and make better choices in the future.
Compatibilists think that as long as we make our choices for our own reasons, we are using free will. This use of free will then does not conflict with the idea that our future is decided by the causally sufficient conditions of our past. The hard determinists would argue that you really never made a choice, that the path you thought you chose for your own reasons was really the only path available due to the causal conditions at the time. That what you perceived as a choice was an illusion, that you could not have made any other choice but the one you did in fact make. By Occam’s razor we should think that what most people report as making free will choices is simpler than that it is an illusion, that choices were not real choices. Thus, it is up to those determinists that maintain that free will is incompatible with determinism to show how this is the case. It is up to these hard determinist type incompatibilists to demonstrate how what we think of as free will is not the reality of the situation. However, the compatibilist’s work is not yet done. There is still a wide gap between the determinism of classical physics and the compatibilist’s notion of free will. In fact, the free will that the compatibilist would claim up to this point is no different than the Libertarian notion of free will. Both the compatibilist and the libertarian believe that we do have free will. That the free will can be constrained by many influences, but we do have real choices that we can make due to our agency and free will.
The libertarian position of free will includes fundamental indeterminism in living systems that organisms can sometimes exploit and other times must actively resist. This indeterminism causes many processes to yield probability rather than certainty. We see this in the sex and genetic makeup of our offspring for example. We also see indeterminism in many mental functions like recalling memories or prioritizing our desires. This libertarian outlook requires that we use trial and error learning which leads to making free willed choices that have some probabilities associated with it. The agency of libertarians comes from what we have learned from the choices we have made in the past. The compatibilist view of free will is that our free will choices may have been determined but that we are oblivious to this predetermination and therefore, we act freely in spite of the fact that we would really only ever have done what we ended up doing. So the situation is that we have all of these factors influencing our choices: genetics, environment, development and other circumstances. The libertarian believes that, in spite of all of these influences, what we have learned can still be a factor in making choices. Whereas, the compatibilist believes that all of these factors determine what choice we make, but because we are not fully cognizant of all of these influences, we freely make the choice that all of these forces add up to. Operationally, both of these give the same results. Both the compatibilist and libertarian act the same, raise their children the same and most likely have the same views of moral responsibility. You can’t really distinguish these two views based on beliefs about free will, although some may think otherwise. The real question has to be, is the living world deterministic or indeterministic. I would say that both sides of this debate have been poorly argued. The libertarian looks at the randomness of mutations and evolution, as well as the probabilities involved in sexual reproduction, and concludes that there is sufficient indeterminism to conclude that determinism in living systems is not valid. The compatibilist responds that the apparent randomness and probabilities arise from our lack of knowledge and not randomness or probability. The determinist looks at our nervous system and cites the “all or none” signal propagation and correlates of consciousness as supporting a deterministic view, while indeterminists look at the molecular basis of neuronal action and neuroplasticity to support their argument.
So we seem to be stuck on building a bridge from determinism to free will with a disagreement as to the nature of living systems being deterministic or indeterministic. Perhaps we should start on the opposite bank where we definitely have determinism in classical physics. Let’s start on the deterministic side and see how far we get. It is hard to argue against determinism in classical physics. This is where philosophers look at colliding billiard balls and falling dominos to come up with the idea that everything is reliably caused such that you can predict the outcome of any event if you have sufficient knowledge of the system and the laws of physics. The hallmark of the deterministic nature of physics is the simple algebraic equations it makes use of in describing the outcome of events. The motions of all Heavenly bodies are explained using some very simple ballistic equations. This leads to a clockwork universe.
From this starting point we must move in the direction of people and sentient animals, because free will, if it exists, would be an advanced biological trait. To get from classical physics to biology requires us first to consider chemistry. In much of chemistry determinism seems to hold up very well. The grouping of individual atoms into substances is explicable by the underlying physics of the atoms. There is chemical potential energy that determines the equilibrium of a chemical system, and many reactions are reversible. However, we do see some indeterminism coming through in the areas of kinetics and thermodynamics. Heat causes molecules in a gas or liquid to exhibit random motion. This random motion gives the impetus for most of the chemical reactions we know about. A whole theory, the Kinetic Molecular Theory, explains how the random motion of molecules cause temperature, pressure and diffusion. These are all caused by the random motion of molecules; however, in most cases the large numbers of molecules involved causes these individual motions and collisions to average out to a definite temperature, pressure and rate of diffusion. So these will not be an impediment to determinism unless the scale we we are looking at is microscopic. The irreversibility of many reactions gives rise to the 2nd law of thermodynamics that not only defines randomness, but also implies that the universe can never return to a previous state. If nothing else, this provides the first time where a scientific law of a system is not derivable from reduction into individual particles. This might be a clue that even if all physical events are deterministic, a system may still contain randomness.
Chemistry contains fundamental indeterminism due to the Kinetic Molecular Theory, statistical mechanics, and the 2nd Law of Thermodynamics. Regardless of how deterministic quantum theory turns out to be, there is randomness in chemistry. There are amorphous solids and crystalline solids. The former has a random arrangement of atoms, the latter has a regular pattern of atoms. Liquids and gases have random molecular motion. This does not mean that the molecules have motion outside the laws of particle physics. It just means that there is no regular pattern or organization as a system. I have heard it said that molecular motion in gases and liquids is deterministic because the molecules move according to Newton’s Laws, even if we can not measure or predict their paths. It is conceivable that they could be measured and defined. Yes, it is in fact conceivable, but is this on point or beside the point? First, let’s be clear as to exactly what we are up against. Gas molecules are not elastic spheres that just bounce off each other. The collisions are inelastic and their shape is irregular and always changing. The cloud of valence electrons on the outside of the molecules is ever changing. The elasticity of the collisions is dependent on exactly where the electrons are at a particular moment in time. The internal vibrations and the spin states of the molecule are quantized and also in a continual state of flux. Thus, we do not have the math to describe what happens when two molecules collide. But an even greater fallacy with thinking the motion of gas and liquid molecules is deterministic, is that conception or prediction implies an observer. What conceivable observer can make use of the fact that the colliding molecules can be predicted by Newtonian physics. Let me explain this bit of philosophy further with an analogous example. Imagine people betting on the flip of the coin. This we agree is a deterministic event governed by classical physics. However, the process could be described as random to an observer if there were no pattern observable other than a 50% chance that the outcome were heads. It doesn’t matter that it is conceivable that a skilled coin flipper could reliably toss heads or tails when they so desired. What matters is if the overall process as observed is fully random, fully determined or if it is at some stochastic middle ground. If all observers agree a process is random, determinism does not apply. So when we move to biology, we should ask ourselves if individual cells observe the process in question as random or do they observe a deterministic process. I seriously doubt the ability of cells to perceive the collision of water molecules, both within and outside the cell, as anything but random.
When we move from the chemical domain to the biological domain, the first question to ask is what is the scale of the system. Is the scale large enough that the indeterminism foundational to chemistry allows us to “average out” the randomness of molecular motion? The cell, the basic building block of all living things, though microscopic, actually contains on the order of 1010 individual water molecules. This seems like a large enough number to average out the random motion of individual molecules. However, many important cellular processes are localized in even smaller organelles and cell membrane receptors that are many orders of magnitude smaller.
The most fundamental process of living cells is keeping the important molecules within the cell but still allowing other molecules and ions to pass through the membrane as needed. This is done at a molecular level where the randomness of molecular motion is quite important. Diffusion, facilitated diffusion, and active transport strategies are used to ensure the correct concentration of most all of the important molecules is maintained within the cell under different environmental conditions. This is what we call homeostasis. Homeostasis is a strategy employed only by living organisms. If not for life, the word and concept of homeostasis would not even exist. Homeostasis is required by cells because cells have to deal with a changing environment. For example, when a bacterium finds itself in an environment that has plenty of glucose, it uses the enzymes that digest glucose to provide the cell with energy. But if the cell moves to an environment that has no glucose but does have lactose, the cell will detect the lactose and start producing the enzymes that break this sugar down to extract energy from it. The perception and reaction of a living cell to its environment is something totally different than the causation found in all of physics. No matter how complex a galaxy is that the physicist studies, they do not have to worry that the stars will change what they are doing because they sense a change in their environment. Planets do not turn off processes due to lack of food or because they sense too many ions are present. Living systems are fundamentally different than any mere physical system.
This directly leads to the catastrophic misunderstanding that determinist philosophers have been suffering from since philosophy was developed by the early Greeks. Living systems have a purpose, nonliving systems do not. All organisms are built around the idea that the organism should survive and reproduce for the continuation of life. Comparing systems without a purpose to a system that has a purpose is not valid. Determinism is not meaningful in systems with a purpose. For one thing the math is different. Classical physics uses simple algebraic and differential equations. Living systems use complex algorithms and Boolean mathematics.
The information is different in living systems. In physics the only information available is directly tied to the object or particle like location, momentum, charge, etc.. In biology all of the objects and particles have this information as well, but there is also stored information in DNA as well. Where did this information that is stored in DNA come from? It can’t come from physics or chemistry because there is no stored repository of information in either of those subjects. This information was arrived at in-deterministically by evolution and can be used as needed by the cell for its purpose of living and reproducing.
Cells build proteins one at a time at sites called ribosomes and these ribosomes are minuscule. Thus, the random motion of molecules makes the process indeterministic. Proteins are built from a nucleic acid template that specifies the exact position and order of the amino acids in the protein. Just as importantly, the process of protein synthesis is highly regulated by the cell. Proteins are synthesized when and if they are needed, and the amount of each protein synthesized is controlled by feedback mechanisms. Feedback mechanisms imply a need to control for random or unexpected deviations. Causation of protein synthesis is a contingent causation. There may need to be 3 or 4 independent factors that must be satisfied to initiate the process.
I find it astounding how philosophers have not yet come to terms with this difference in causation in living systems as opposed to physical processes. Philosophers give examples of determinism like falling dominos and colliding billiard balls and then feel no shame in saying that genetics causes behavior in a similar fashion. The causation is fundamentally different. If you can not see this, you can’t be much of a philosopher. Determinist philosophers must be forced to explain in detail how cause and effect works in living systems with contingent causation and in light of the random processes of diffusion, mutation, and sexual reproduction. Most relevant to free will would be explaining the function at the neuronal synapse junctions. These are only about 100 water molecules wide, which means that the indeterminate processes of diffusion and receptor binding must be accounted for. Also, the propagation of a signal by associative neurons is through a contingent mechanism like what was described for protein synthesis, but to an even greater degree. Neuroscientist, Peter Tse, has termed causation of neuronal propagation as criteria causation. He gives many examples of how neurons are constantly resetting the criteria of neural propagation based on different factors happening throughout the brain. This he concludes only works in an indeterministic system.
So in going back to the bridge building analogy, compatibilism is not very objectionable to libertarians when discussing free will and not very objectionable to determinists when describing the nature of the universe. But unfortunately, compatibilists do not ever bridge the explanatory gap to get free will through deterministic causation. The libertarian intuition of indeterministic causation being needed for free will seems the most plausible at the current time. I have not fully explained the mechanism of how we obtain and use free will within an indeterministic framework here. But I have previously written on that very topic here:
“The Mechanism of Free Will” and in my book here: “What Determined the Warthog?”
submitted by Rthadcarr1956 to freewill [link] [comments]
I analogize compatibilism to building a bridge starting on the opposite banks of a river. It is easy to get started on either side, but the real trick is to get them to meet in the middle. So on one bank of the river you have this deterministic view where classical physics is obviously deterministic and on the opposite shore you have free willed actions of the individual. The trick is to connect the two while not contradicting either one. Let’s begin with the idea of free will. Free will is the default position that most everyone operates under. Free will means that in many situations we have a limited freedom to choose between different options. We can decide when to turn right or go straight, when to go to work and when to stay home, and the whole panoply of choices we make every day. We often reflect on the important choices we make and evaluate how good of a choice we made. Not that we can go back and change things, but we can learn and make better choices in the future.
Compatibilists think that as long as we make our choices for our own reasons, we are using free will. This use of free will then does not conflict with the idea that our future is decided by the causally sufficient conditions of our past. The hard determinists would argue that you really never made a choice, that the path you thought you chose for your own reasons was really the only path available due to the causal conditions at the time. That what you perceived as a choice was an illusion, that you could not have made any other choice but the one you did in fact make. By Occam’s razor we should think that what most people report as making free will choices is simpler than that it is an illusion, that choices were not real choices. Thus, it is up to those determinists that maintain that free will is incompatible with determinism to show how this is the case. It is up to these hard determinist type incompatibilists to demonstrate how what we think of as free will is not the reality of the situation. However, the compatibilist’s work is not yet done. There is still a wide gap between the determinism of classical physics and the compatibilist’s notion of free will. In fact, the free will that the compatibilist would claim up to this point is no different than the Libertarian notion of free will. Both the compatibilist and the libertarian believe that we do have free will. That the free will can be constrained by many influences, but we do have real choices that we can make due to our agency and free will.
The libertarian position of free will includes fundamental indeterminism in living systems that organisms can sometimes exploit and other times must actively resist. This indeterminism causes many processes to yield probability rather than certainty. We see this in the sex and genetic makeup of our offspring for example. We also see indeterminism in many mental functions like recalling memories or prioritizing our desires. This libertarian outlook requires that we use trial and error learning which leads to making free willed choices that have some probabilities associated with it. The agency of libertarians comes from what we have learned from the choices we have made in the past. The compatibilist view of free will is that our free will choices may have been determined but that we are oblivious to this predetermination and therefore, we act freely in spite of the fact that we would really only ever have done what we ended up doing. So the situation is that we have all of these factors influencing our choices: genetics, environment, development and other circumstances. The libertarian believes that, in spite of all of these influences, what we have learned can still be a factor in making choices. Whereas, the compatibilist believes that all of these factors determine what choice we make, but because we are not fully cognizant of all of these influences, we freely make the choice that all of these forces add up to. Operationally, both of these give the same results. Both the compatibilist and libertarian act the same, raise their children the same and most likely have the same views of moral responsibility. You can’t really distinguish these two views based on beliefs about free will, although some may think otherwise. The real question has to be, is the living world deterministic or indeterministic. I would say that both sides of this debate have been poorly argued. The libertarian looks at the randomness of mutations and evolution, as well as the probabilities involved in sexual reproduction, and concludes that there is sufficient indeterminism to conclude that determinism in living systems is not valid. The compatibilist responds that the apparent randomness and probabilities arise from our lack of knowledge and not randomness or probability. The determinist looks at our nervous system and cites the “all or none” signal propagation and correlates of consciousness as supporting a deterministic view, while indeterminists look at the molecular basis of neuronal action and neuroplasticity to support their argument.
So we seem to be stuck on building a bridge from determinism to free will with a disagreement as to the nature of living systems being deterministic or indeterministic. Perhaps we should start on the opposite bank where we definitely have determinism in classical physics. Let’s start on the deterministic side and see how far we get. It is hard to argue against determinism in classical physics. This is where philosophers look at colliding billiard balls and falling dominos to come up with the idea that everything is reliably caused such that you can predict the outcome of any event if you have sufficient knowledge of the system and the laws of physics. The hallmark of the deterministic nature of physics is the simple algebraic equations it makes use of in describing the outcome of events. The motions of all Heavenly bodies are explained using some very simple ballistic equations. This leads to a clockwork universe.
From this starting point we must move in the direction of people and sentient animals, because free will, if it exists, would be an advanced biological trait. To get from classical physics to biology requires us first to consider chemistry. In much of chemistry determinism seems to hold up very well. The grouping of individual atoms into substances is explicable by the underlying physics of the atoms. There is chemical potential energy that determines the equilibrium of a chemical system, and many reactions are reversible. However, we do see some indeterminism coming through in the areas of kinetics and thermodynamics. Heat causes molecules in a gas or liquid to exhibit random motion. This random motion gives the impetus for most of the chemical reactions we know about. A whole theory, the Kinetic Molecular Theory, explains how the random motion of molecules cause temperature, pressure and diffusion. These are all caused by the random motion of molecules; however, in most cases the large numbers of molecules involved causes these individual motions and collisions to average out to a definite temperature, pressure and rate of diffusion. So these will not be an impediment to determinism unless the scale we we are looking at is microscopic. The irreversibility of many reactions gives rise to the 2nd law of thermodynamics that not only defines randomness, but also implies that the universe can never return to a previous state. If nothing else, this provides the first time where a scientific law of a system is not derivable from reduction into individual particles. This might be a clue that even if all physical events are deterministic, a system may still contain randomness.
Chemistry contains fundamental indeterminism due to the Kinetic Molecular Theory, statistical mechanics, and the 2nd Law of Thermodynamics. Regardless of how deterministic quantum theory turns out to be, there is randomness in chemistry. There are amorphous solids and crystalline solids. The former has a random arrangement of atoms, the latter has a regular pattern of atoms. Liquids and gases have random molecular motion. This does not mean that the molecules have motion outside the laws of particle physics. It just means that there is no regular pattern or organization as a system. I have heard it said that molecular motion in gases and liquids is deterministic because the molecules move according to Newton’s Laws, even if we can not measure or predict their paths. It is conceivable that they could be measured and defined. Yes, it is in fact conceivable, but is this on point or beside the point? First, let’s be clear as to exactly what we are up against. Gas molecules are not elastic spheres that just bounce off each other. The collisions are inelastic and their shape is irregular and always changing. The cloud of valence electrons on the outside of the molecules is ever changing. The elasticity of the collisions is dependent on exactly where the electrons are at a particular moment in time. The internal vibrations and the spin states of the molecule are quantized and also in a continual state of flux. Thus, we do not have the math to describe what happens when two molecules collide. But an even greater fallacy with thinking the motion of gas and liquid molecules is deterministic, is that conception or prediction implies an observer. What conceivable observer can make use of the fact that the colliding molecules can be predicted by Newtonian physics. Let me explain this bit of philosophy further with an analogous example. Imagine people betting on the flip of the coin. This we agree is a deterministic event governed by classical physics. However, the process could be described as random to an observer if there were no pattern observable other than a 50% chance that the outcome were heads. It doesn’t matter that it is conceivable that a skilled coin flipper could reliably toss heads or tails when they so desired. What matters is if the overall process as observed is fully random, fully determined or if it is at some stochastic middle ground. If all observers agree a process is random, determinism does not apply. So when we move to biology, we should ask ourselves if individual cells observe the process in question as random or do they observe a deterministic process. I seriously doubt the ability of cells to perceive the collision of water molecules, both within and outside the cell, as anything but random.
When we move from the chemical domain to the biological domain, the first question to ask is what is the scale of the system. Is the scale large enough that the indeterminism foundational to chemistry allows us to “average out” the randomness of molecular motion? The cell, the basic building block of all living things, though microscopic, actually contains on the order of 1010 individual water molecules. This seems like a large enough number to average out the random motion of individual molecules. However, many important cellular processes are localized in even smaller organelles and cell membrane receptors that are many orders of magnitude smaller.
The most fundamental process of living cells is keeping the important molecules within the cell but still allowing other molecules and ions to pass through the membrane as needed. This is done at a molecular level where the randomness of molecular motion is quite important. Diffusion, facilitated diffusion, and active transport strategies are used to ensure the correct concentration of most all of the important molecules is maintained within the cell under different environmental conditions. This is what we call homeostasis. Homeostasis is a strategy employed only by living organisms. If not for life, the word and concept of homeostasis would not even exist. Homeostasis is required by cells because cells have to deal with a changing environment. For example, when a bacterium finds itself in an environment that has plenty of glucose, it uses the enzymes that digest glucose to provide the cell with energy. But if the cell moves to an environment that has no glucose but does have lactose, the cell will detect the lactose and start producing the enzymes that break this sugar down to extract energy from it. The perception and reaction of a living cell to its environment is something totally different than the causation found in all of physics. No matter how complex a galaxy is that the physicist studies, they do not have to worry that the stars will change what they are doing because they sense a change in their environment. Planets do not turn off processes due to lack of food or because they sense too many ions are present. Living systems are fundamentally different than any mere physical system.
This directly leads to the catastrophic misunderstanding that determinist philosophers have been suffering from since philosophy was developed by the early Greeks. Living systems have a purpose, nonliving systems do not. All organisms are built around the idea that the organism should survive and reproduce for the continuation of life. Comparing systems without a purpose to a system that has a purpose is not valid. Determinism is not meaningful in systems with a purpose. For one thing the math is different. Classical physics uses simple algebraic and differential equations. Living systems use complex algorithms and Boolean mathematics.
The information is different in living systems. In physics the only information available is directly tied to the object or particle like location, momentum, charge, etc.. In biology all of the objects and particles have this information as well, but there is also stored information in DNA as well. Where did this information that is stored in DNA come from? It can’t come from physics or chemistry because there is no stored repository of information in either of those subjects. This information was arrived at in-deterministically by evolution and can be used as needed by the cell for its purpose of living and reproducing.
Cells build proteins one at a time at sites called ribosomes and these ribosomes are minuscule. Thus, the random motion of molecules makes the process indeterministic. Proteins are built from a nucleic acid template that specifies the exact position and order of the amino acids in the protein. Just as importantly, the process of protein synthesis is highly regulated by the cell. Proteins are synthesized when and if they are needed, and the amount of each protein synthesized is controlled by feedback mechanisms. Feedback mechanisms imply a need to control for random or unexpected deviations. Causation of protein synthesis is a contingent causation. There may need to be 3 or 4 independent factors that must be satisfied to initiate the process.
I find it astounding how philosophers have not yet come to terms with this difference in causation in living systems as opposed to physical processes. Philosophers give examples of determinism like falling dominos and colliding billiard balls and then feel no shame in saying that genetics causes behavior in a similar fashion. The causation is fundamentally different. If you can not see this, you can’t be much of a philosopher. Determinist philosophers must be forced to explain in detail how cause and effect works in living systems with contingent causation and in light of the random processes of diffusion, mutation, and sexual reproduction. Most relevant to free will would be explaining the function at the neuronal synapse junctions. These are only about 100 water molecules wide, which means that the indeterminate processes of diffusion and receptor binding must be accounted for. Also, the propagation of a signal by associative neurons is through a contingent mechanism like what was described for protein synthesis, but to an even greater degree. Neuroscientist, Peter Tse, has termed causation of neuronal propagation as criteria causation. He gives many examples of how neurons are constantly resetting the criteria of neural propagation based on different factors happening throughout the brain. This he concludes only works in an indeterministic system.
So in going back to the bridge building analogy, compatibilism is not very objectionable to libertarians when discussing free will and not very objectionable to determinists when describing the nature of the universe. But unfortunately, compatibilists do not ever bridge the explanatory gap to get free will through deterministic causation. The libertarian intuition of indeterministic causation being needed for free will seems the most plausible at the current time. I have not fully explained the mechanism of how we obtain and use free will within an indeterministic framework here. But I have previously written on that very topic here:
“The Mechanism of Free Will” and in my book here: “What Determined the Warthog?”
2024.03.26 19:20 dr_snif Literature Review: Stepwise formation of the bacterial flagellar system
This paper has been tossed around in series of deranged creationist posts without, in my opinion, any thorough review of the actual data in any of the posts. For those interested I'm presenting a review, with as much academic rigor as possible while trying to maintain clarity for lay people in the sub.
I'd like to start with why I think I'm qualified to address this: BSc in Microbiology (Math and Biophysics minors), and PhD in Biomedical Engineering (Developmental Biomechanics). I've done bacteriology research, as well as research on the evolutionary and developmental aspects of organ and tissue development/mechanics. This will be relatively long, so I apologize. I will summarize each section (Intro, methods and results) of the paper.
Introduction
Flagella are complex organelles with distinct structures, and around 24 structural proteins had been identified across several species at the time of publication (2007). These proteins make substructures such as a basal body, motor, switch, hook, filament and export apparatus. There is broad variety in specific flagellar structure across species, but specific proteins share broad homology - indicating common ancestry. Not much was known at the time about the specific phylogenetic (the hierarchical lineage of protein evolution) relationships between these proteins at the time. Based on structural similarities with other membrane-bound proteins, it seemed that these proteins were derived from some sort of proton-based secretion-system - and shows strong homology with Type-3 Secretion System (TTSS) - indicating common ancestry. So, flagella and TTSS share common ancestry - although flagella likely arose earlier.
Methods
The authors obtained genome data from 41 unique genus of bacteria all containing flagella from 11 higher order phyla from published genome databases (KEGG). They then performed phylogenetic profiling on these 41 genomes. They various BLAST techniques to identify orthologs between the species (proteins that are found in all species, that serve the same or very similar function and is derived from a common ancestor). Orthologous genes/proteins help identify phylogenetic relationships based on differences in their sequences. Closely related genes are more similar, distantly related genes are less similar. They used flagellar proteins from a few species to make sure they get as many orthologs as possible.
They then quantified similarity between core proteins within each species. They performed phylogenetic analysis on the flagellar proteins. Amino acid sequence homology was used to determine relatedness of proteins and generate most likely phylogenetic trees (these show which proteins would evolve earlier, and relationships with newer proteins - much like the tree of life). They then compare each protein to 14 proteins that are present in all flagellar systems (these would have been present from the earlier parts of evolution since they are present in all species.)
They also develop a bacterial species tree using alignments of ribosomal proteins (present in all domains of life), very similar to the previous analysis.
Results
They identify and classify all core proteins based on their function and presence in different species. This is summarized in Figure 1. This gives us an idea of the protein orthologs between the species, and which species have what specific components. Not particularly interesting for the evolution - but useful for understanding the system and its diversity among species, as well as identifying the structural components of the flagella.
They then compare the phylogenetic trees generated by flagellar protein homology and homology of ribosomal proteins. This comparison is meant to show that based on the assumption of evolution - the evolutionary patterns of the flagellar proteins, and the evolutionary patterns of the bacterial species based on ribosomal proteins agree with each other - except for some incongruencies based on horizontal gene transfers (boxed species Figure 2). Horizontal gene transfers are events where different closely species share genes between each other. This is different from traditional evolution which includes vertical gene transfer by cell division within the same species. This strongly suggests that flagellar proteins evolved along with the bacterial species in the same order.
Figure 3 shows the homology relationships between core proteins. The links and the number show how many species share homology between these two genes. They identified 10 genes with really high rates of homology - indicating these were generated by duplication events - and all represent extracellular parts of the flagellum. This is based on E. coli flagellar complex. They then also analyzed similarities based on the other species' genomes and found further homology between core flagellar proteins. Flagellar proteins had very low homology with non-flagellar proteins except for a few (mostly related to secretion system proteins). Combining these analyses, the authors develop detailed phylogenetic trees of these core proteins (Supplementary Figures 5a,b).
Discussion
submitted by dr_snif to DebateEvolution [link] [comments]
I'd like to start with why I think I'm qualified to address this: BSc in Microbiology (Math and Biophysics minors), and PhD in Biomedical Engineering (Developmental Biomechanics). I've done bacteriology research, as well as research on the evolutionary and developmental aspects of organ and tissue development/mechanics. This will be relatively long, so I apologize. I will summarize each section (Intro, methods and results) of the paper.
Introduction
Flagella are complex organelles with distinct structures, and around 24 structural proteins had been identified across several species at the time of publication (2007). These proteins make substructures such as a basal body, motor, switch, hook, filament and export apparatus. There is broad variety in specific flagellar structure across species, but specific proteins share broad homology - indicating common ancestry. Not much was known at the time about the specific phylogenetic (the hierarchical lineage of protein evolution) relationships between these proteins at the time. Based on structural similarities with other membrane-bound proteins, it seemed that these proteins were derived from some sort of proton-based secretion-system - and shows strong homology with Type-3 Secretion System (TTSS) - indicating common ancestry. So, flagella and TTSS share common ancestry - although flagella likely arose earlier.
Methods
The authors obtained genome data from 41 unique genus of bacteria all containing flagella from 11 higher order phyla from published genome databases (KEGG). They then performed phylogenetic profiling on these 41 genomes. They various BLAST techniques to identify orthologs between the species (proteins that are found in all species, that serve the same or very similar function and is derived from a common ancestor). Orthologous genes/proteins help identify phylogenetic relationships based on differences in their sequences. Closely related genes are more similar, distantly related genes are less similar. They used flagellar proteins from a few species to make sure they get as many orthologs as possible.
They then quantified similarity between core proteins within each species. They performed phylogenetic analysis on the flagellar proteins. Amino acid sequence homology was used to determine relatedness of proteins and generate most likely phylogenetic trees (these show which proteins would evolve earlier, and relationships with newer proteins - much like the tree of life). They then compare each protein to 14 proteins that are present in all flagellar systems (these would have been present from the earlier parts of evolution since they are present in all species.)
They also develop a bacterial species tree using alignments of ribosomal proteins (present in all domains of life), very similar to the previous analysis.
Results
They identify and classify all core proteins based on their function and presence in different species. This is summarized in Figure 1. This gives us an idea of the protein orthologs between the species, and which species have what specific components. Not particularly interesting for the evolution - but useful for understanding the system and its diversity among species, as well as identifying the structural components of the flagella.
They then compare the phylogenetic trees generated by flagellar protein homology and homology of ribosomal proteins. This comparison is meant to show that based on the assumption of evolution - the evolutionary patterns of the flagellar proteins, and the evolutionary patterns of the bacterial species based on ribosomal proteins agree with each other - except for some incongruencies based on horizontal gene transfers (boxed species Figure 2). Horizontal gene transfers are events where different closely species share genes between each other. This is different from traditional evolution which includes vertical gene transfer by cell division within the same species. This strongly suggests that flagellar proteins evolved along with the bacterial species in the same order.
Figure 3 shows the homology relationships between core proteins. The links and the number show how many species share homology between these two genes. They identified 10 genes with really high rates of homology - indicating these were generated by duplication events - and all represent extracellular parts of the flagellum. This is based on E. coli flagellar complex. They then also analyzed similarities based on the other species' genomes and found further homology between core flagellar proteins. Flagellar proteins had very low homology with non-flagellar proteins except for a few (mostly related to secretion system proteins). Combining these analyses, the authors develop detailed phylogenetic trees of these core proteins (Supplementary Figures 5a,b).
Discussion
- Identified 24 core flagellar proteins
- Sequence homology between these proteins indicate common ancestry through duplications (paralogous)
- Protein phylogeny is mostly congruent with bacterial phylogeny (except for gene transfer events)
- These core proteins diversified before the shared ancestor of Bacteria
- Phylogeny of these core proteins reveal paralogous relationships derived from gene duplication
- Order of protein evolution matches previous hypothesis of inside-out assembly of flagella
- Inner components appear first in phylogeny, outer components appear later
- Order of assembly is same as evolutionary history - analogous to embryonic development of animals
- Core protein homologies show the phylogenetic relationship between specific core proteins with high homology (earliest appearing flagellar genes)
- Overall, this paper uses the concepts of homology to identify phylogenetic relationships between flagellar evolution which mimics the inside-out assembly of the flagella.
- My opinions:
- The fact that evolution and assembly follow the same sequence is highly compelling.
- Secretions systems with added extracellular components (even if short), would increase fitness of the bacteria since it would provide advantages immediately - chemosensing, or adherence to surroundings
- Same principle for motor components - movements within the extracellular flagellar components would improve fitness by improving motility (even if marginally)
- Congruence between bacterial evolution and flagellar protein evolution is very compelling.
2024.02.02 15:41 Silly_Bad_1804 Pele, a world with no star. Against all odds a true biosphere has established itself and with it, the Kapnozoic Eon is coming to an end. But how did we get here?
 | submitted by Silly_Bad_1804 to u/Silly_Bad_1804 [link] [comments] |
2023.04.12 18:19 achoiceofthree Found Chef from South Park in Rau's Sc and Tech Compass. XD
 | submitted by achoiceofthree to UPSC [link] [comments] |
2022.11.04 07:41 Chas-- (6) All the Science of Bonding - From Inorganic, to Organic, to Biochemistry - Has Holes and Requires Faith (Dr. Yes!)
Now, speaking of faith, you have to trust me in this series, I am actually building towards a point, but it will take a lot of construction to get to where I believe we are headed, hang in there for a cosmic surprise ending.
That is Chemistry and it requires faith, since Chemistry is just applied Physics which has gaps, holes and is abundantly incomplete since it uses mathematical models of nature with little explanatory power (we trust that their predictive nature means that they are correct, while remaining ignorant as to why or how.) And earlier in my fourth posting. I summarized why logical systems containing a "small amount of arithmetic" such as mathematics, are incomplete according to Torkel Franzén's writings on Gödel's Incompleteness Theorems I and II. The tedious formal proofs of Gödel's Incompleteness Theorems by Hilbert and Bernays don't explain much either.
As the vampire in Fright Night says to Roddy McDowell holding up a cross with shaking hands, "You have to have faith for that to work!" (It's not a James Bond quote, but I couldn't resist.)
In that fifth posting, I mentioned in discussing Quantum Mechanics (QM) that entanglement involves superposition (you can think of this as uncertainty in position and momentum of low-mass particles like electrons), the no-cloning rule (which means no observed information or energy coming in or going out of the entangled system), teleportation (which means that those uncertain particles can change position instantly and tunnel through barriers), that those entangled systems have constant entropy (which I will describe next), and the instantaneous collapse (even across vast distances) of entanglement's wave function through the phenomenon called decoherence, which will most likely never be observable and understood scientifically.
Another way to look at entropy is that the total energy put into an engine does not end up in the work output by that engine. Some of it is irreversibly lost as waste heat and some irreversibly goes into wear and tear on the engine itself. That gradually disordered engine will eventually wear out and produce less work, as it wears out. This also happens to living beings over time. :^(
In the late 19th century, Ludwig Boltzmann found that entropy) was related to the logarithm of the total number of microstates (identified by the omega symbol Ω) of the system and statistical thermodynamics was born:
s = kB ln Ω [where kB is the Boltzmann constant and is fundamental.]
A simple way to think about Boltzmann entropy, is that the greater the number of microstates in the system, the greater the entropy, but only growing at the logarithmic rate. Using the aging engine example, the old engine has a variety of new states of operation: it smokes, rattles, vibrates and produces more different kinds of noise and increasingly less work than when it was new. Just like we do as we get older.
The other 20% of the air you breath is double-bonded dioxygen and that is a 4 to 1 ratio of dnitrogen to dioxygen in the atmosphere. In the watery surface of your lung, however, due to the inertness of dinitrogen and the partial polarity of dioxygen and its hydrogen bonding to water, dioxygen dissolves at a ratio of 2 to 1 over dinitrogen. So the colliding air molecules flow in through the mean free path statistically, but when the air molecules hit the watery surface of the lung, the dinitrogen is 8 times as likely to bounce out over dioxygen, making the water in your lung a chemical concentrator for oxygen. OSHA, by the way declares anything over 80% dnitrogen or under 19% dioxygen to be hazardous, and also OSHA declares that levels above 23.5% dioxygen to be hazardous to the alveoli of lungs over time), so our kind of life, that breathes air is quite finely balanced.
In physical chemistry, reactions accomplish their transitions by having reversibility up until the presence of a form of the incoming reactants called an "activated complex", which proceeds to drive the energy of the system over the required energy hump and to the lower energy state of the products of the reaction.
Reaction rates are ruled by the slow step in a chain of reaction transitions, and each transition can have its reaction rate sped up by the use of catalysts that participate but remain available in the system to mediate the next transition of an activated complex into products.
Interestingly, gas phase reactions ARE mostly reversible in the physical world, outside of the lab or the production facility at the chemical plant, where we coerce processes to move in certain productive and profitable directions.
This is why the search for life by telescopes of varying kinds is always a search for what the NASA scientists call the "water hole" which is now considered a necessary piece of evidence of extraterrestrial life in the universe.
So, you never see messenger RNA spooling backwards out of a ribosome and turning protein into amino acids. Protein transcription only moves in the forward direction from amino acids transcribing messenger RNA at the ribosome like a tape reader and spooling off protein chains, entirely due to the reaction occurring in aqueous (watery) solution where there is a well-regulated and thoroughly cool enough environment to prevent local heating from undoing nature's work.
Max says that when photons "scan" through non-living matter the entropy increases. However, when photons "scan" through living matter, the entropy decreases. Living things respond to external stimuli and evolve, react and learn accordingly. Living things evolve by becoming more complex in a highly ordered and genetically remembered way, and the most ordered (lowest entropy) living organ (or frankly, system of any kind) is the nervous system and the brain. And the most complex and ordered system that we know of in the universe is the human brain, which is more like an analog switching system and not digital at all: there are no registers, just nerve cells interacting with the voltage differences created in axon/dendrite switching networks.
A fruit fly brain has 20 million synaptic connections, but a human brain has 100 trillion connections all firing and changing neural voltages even when we sleep. One could argue that makes for a lot of moving parts and higher entropy (s = kB ln Ω), however that brain has effectively one state (Ω=1) and that is your consciousness, and the natural log of one is zero: an astonishingly low entropy.
Also, there is no "small amount of arithmetic" because there is no integer or floating point unit, the brain emulates those digital systems in the gray matter with vastly slower performance than your typical calculator.
Hence we living systems with brains are capable of formal logic proving our theorems to be true according to Gödel's Completeness Theorem, whereas digital systems which use a "small amount of arithmetic" just to find each instruction address, memory register and virtual address are permanently restricted to following Gödel's Incompleteness Theorems I and II. So, we should stop worrying about the coming digital supremacy over humans, or any other living beings, for that matter. Computers cannot deduce with strong logic, they can only induce with weak logic. A robot can kill you, but a human programmer will have engineered your demise, either intentionally or by neglect. Robots will never be certain of the difference between what is right and what is wrong. We can have faith and make reasoned decisions based on it.
Interestingly, there are six times as much processed logical visual signals flowing through the thalamus from the visual cortex as the original raw physical visual flow from the optic nerves. This explains why those people you see walking down the street having a conversation without a cell phone are really seeing someone they are talking to. Their echoes from the past are replaying from the visual cortex and appear as real as the raw optical flow, maybe even more real.
What I perceive when I chant to the Gohonzon arises entirely from inside me. What a digital system sees when it looks at the Gohonzon will not likely ever arise from inside, it will arise from code, once again, written by a human programmer, or generated by a machine programmed by a human programmer.
I give you Abraham Lincoln as proof of the permanent supremacy of living beings over the inanimate. He demonstrates the difference between (1) the imperfect expedient means employed by all the Buddhas to steadily improve the lives of living beings, and (2) the impractical and impossible perfection of thought, word and deed. No machine will ever get this right.
Describing Lincoln, historian Jon Meacham notes that there were three critical moments that reflected his principles while employing the expedient means of his Presidency, which always bent towards the direction of the Declaration of Independence as his personal compass:
With the same kind of faith that Lincoln had in the better angels of human nature, we will also navigate through the current river of storms to reach the 2030 Centennial of the SGI. Even if individually, some of us don't make it through to the promised land of 2030.
Of course, that would depend on the noblesse oblige of Bianca ProMAGA and the SGI Whisperers kindly allowing us to continue doing Kosen Rufu.
submitted by Chas-- to SGIWhistleblowersMITA [link] [comments]
Previously ...
In my fifth posting, I summarized the mechanism (Kinetic Gas Theory, Mean-Free Path) that allows air to occupy a partial vacuum: such as that produced by your lungs, thereby allowing you to live for a few minutes more. It is the same mechanism that allows planes to fly, originally called Bernoulli's Principle, but not explained at all by Bernoulli back in the day.Speaking of bonding, from Moonraker:What I did not summarize in the last posting is how that mean-free path action allows you to live, because gas flow is necessary, but insufficient for life.
Hugo Drax aboard the space station: (Hastily grabs pistol, trains it on Bond who has cornered him) At least I shall have the pleasure of putting you out of my misery, Mr. Bond.
(Drax chuckles as Bond raises his hands)
Hugo Drax : Desolated, Mr. Bond?
Bond : (Bond shoots Drax with a poison dart from his wrist-gun. Drax, gasping, drops his pistol and staggers backwards toward the airlock) Heartbroken, Mr. Drax. Allow me.
(He opens the airlock door and pushes Drax in)
Bond : Take a giant step for mankind!
(He closes the door and ejects Drax into space)
Dr. Holly Goodhead : (rejoining 007) Where's Drax?
Bond : Oh, he had to fly.
That is Chemistry and it requires faith, since Chemistry is just applied Physics which has gaps, holes and is abundantly incomplete since it uses mathematical models of nature with little explanatory power (we trust that their predictive nature means that they are correct, while remaining ignorant as to why or how.) And earlier in my fourth posting. I summarized why logical systems containing a "small amount of arithmetic" such as mathematics, are incomplete according to Torkel Franzén's writings on Gödel's Incompleteness Theorems I and II. The tedious formal proofs of Gödel's Incompleteness Theorems by Hilbert and Bernays don't explain much either.
As the vampire in Fright Night says to Roddy McDowell holding up a cross with shaking hands, "You have to have faith for that to work!" (It's not a James Bond quote, but I couldn't resist.)
In that fifth posting, I mentioned in discussing Quantum Mechanics (QM) that entanglement involves superposition (you can think of this as uncertainty in position and momentum of low-mass particles like electrons), the no-cloning rule (which means no observed information or energy coming in or going out of the entangled system), teleportation (which means that those uncertain particles can change position instantly and tunnel through barriers), that those entangled systems have constant entropy (which I will describe next), and the instantaneous collapse (even across vast distances) of entanglement's wave function through the phenomenon called decoherence, which will most likely never be observable and understood scientifically.
What is entropy?
Simply put, entropy (quantified as "s") is the measure of a particular kind of order (s is then smaller) and disorder (s is then larger) for any system. Closed systems have entropy that is always increasing (ds >= 0, which means the differential change in s is non-negative and s is never decreasing), and that implies that the components of those systems will exchange entropy while the total stays fairly constant (a reversible process, like moving something) or increases (an irreversible process, like breaking and frying an egg.)Another way to look at entropy is that the total energy put into an engine does not end up in the work output by that engine. Some of it is irreversibly lost as waste heat and some irreversibly goes into wear and tear on the engine itself. That gradually disordered engine will eventually wear out and produce less work, as it wears out. This also happens to living beings over time. :^(
From Goldfinger:Entropy originally was identified by Rudolf Clausius in the studies of heat produced in boring the barrels of cannon in late 18th century Britain by Count Rumford. Heat was produced by friction and the boring tools wore out. So many plowshares wrought from the swords of war science!
Q: "..reception on the dashboard here. Audio-visual, range a hundred and fifty miles."
Bond: "Ingenious, and useful too. Allow a man to stop off for a quick one en route."
Q: "It has not been perfected, out of years of patient research, entirely for that purpose, 007. And incidentally, we'd appreciate its return, along with all your other equipment, intact for once, when you return from the field."
Bond: "Well, you'd be surprised the amount of wear and tear that goes on out there in the field."
In the late 19th century, Ludwig Boltzmann found that entropy) was related to the logarithm of the total number of microstates (identified by the omega symbol Ω) of the system and statistical thermodynamics was born:
s = kB ln Ω [where kB is the Boltzmann constant and is fundamental.]
A simple way to think about Boltzmann entropy, is that the greater the number of microstates in the system, the greater the entropy, but only growing at the logarithmic rate. Using the aging engine example, the old engine has a variety of new states of operation: it smokes, rattles, vibrates and produces more different kinds of noise and increasingly less work than when it was new. Just like we do as we get older.
Entangled Systems Are Different (et vive la différence!)
However, for entangled systems, which are closed and not interacting with the environment (no cloning) until decoherence collapses the wave function: while still entangled, the entropy is constant and NOT increasing (ds = 0) unlike closed systems that are not entangled. So, atoms with spin-paired electrons in entangled atomic orbitals and molecules with spin-paired electrons in entangled molecular bonding orbitals constructed of atomic orbitals ... those little entangled engines of chemistry don't run down and wear out, as in the covalent bonding in diamonds.From Diamonds Are Forever:The strongest chemical bond in the universe is actually not the diamond carbon to carbon sp3 single tetrahedral crystal bonds, first prize goes to the dinitrogen triple bond present in 80% of our atmosphere, which can be enhanced artificially by adding strong polarizing atoms on the ends of the two nitrogen atoms connected by the triple bond. Called "protonation" by hydrogen or fluorine, this draws charge away from the triple bond and lowers the energy of the bonding orbitals: to win the prize as the strongest bond known to science.
Felix Leiter: I give up. I know the diamonds are in the body, but where?
Bond: Alimentary, Dr. Leiter...
- See the figure 9.28 text in this book below explaining bonding orbitals (lower energy) and antibonding orbitals (higher energy) and why these covalent molecular orbital bonds are so strong). (This is quite an excellent Creative Commons general chemistry textbook, I must say, better than the Dickerson, Gray and Haight Chemical Principles that I studied back in the day, and it also includes a chunk of the Physical Chemistry by Barrow, and the molecular orbital theory from Inorganic Chemistry by Huheey that I studied as well.)
- See the little chart with the numbers in the abstract of an article specifically on this phenomenon.
From Die Another Day:You can tell the dinitrogen bond is strong, because of the intense higher frequency (frequency ν is linear to energy: E=hν) blue light that it scatters from the sun, which is why the sky is blue. The phenomenon is called Rayleigh Scattering, and the blue light is scattered at a right angle to the light coming from the sun, which is why why the morning and evening sun make such a deep blue sky straight above you. If you put your fist up blocking the sun (never, ever look at the sun directly) you will notice that the area around the sun is not very blue and that is because it's hard to make that bank shot in a straight line. Interestingly, metallic gold (Au) absorbs all the blue light from incandescent sources, like the sun and the blue sky, reflecting the remaining unique golden color that remains after blue is subtracted, so beloved by many.
Bond: (after he gives Col. Moon the briefcase full of diamonds, rigged with explosives) Don't blow it all at once.
From Goldfinger:However, that inertness of atmospheric dinitrogen also allows you to breath and live, if you have a little faith and open your mouth to let the air flow in along the mean free path into the partial vacuum of your lungs (fully described in my last posting about halfway down here).
Goldfinger shows off his industrial laser by having it slowly track toward Bond, lying supine and lashed to slab of gold.
Goldfinger: This is gold, Mr Bond. All my life, I have been in love with its color, its brilliance, its divine heaviness. I welcome any enterprise that will increase my stock- which is considerable.
Bond: I think you've made your point, Goldfinger. Thank you for the demonstration.
Goldfinger: Choose your next witticism carefully, Mr Bond — it may be your last. The purpose of our two previous encounters is now very clear to me. I do not intend to be disturbed by another. Goodnight, Mr Bond. (leaves Bond to the tracking laser)
Bond: Do you expect me to talk?
Goldfinger: (looks back, laughing) No, Mr Bond, I expect you to die!
The other 20% of the air you breath is double-bonded dioxygen and that is a 4 to 1 ratio of dnitrogen to dioxygen in the atmosphere. In the watery surface of your lung, however, due to the inertness of dinitrogen and the partial polarity of dioxygen and its hydrogen bonding to water, dioxygen dissolves at a ratio of 2 to 1 over dinitrogen. So the colliding air molecules flow in through the mean free path statistically, but when the air molecules hit the watery surface of the lung, the dinitrogen is 8 times as likely to bounce out over dioxygen, making the water in your lung a chemical concentrator for oxygen. OSHA, by the way declares anything over 80% dnitrogen or under 19% dioxygen to be hazardous, and also OSHA declares that levels above 23.5% dioxygen to be hazardous to the alveoli of lungs over time), so our kind of life, that breathes air is quite finely balanced.
The Argument Regarding Reversible Versus Irreversible In QM
There is an argument between physicists and chemists regarding quantum mechanics where the physicists say that QM processes are totally reversible and chemists argue that there is a punctuated equilibrium of reversibility in complex chemical and especially biochemical processes regarding life.In physical chemistry, reactions accomplish their transitions by having reversibility up until the presence of a form of the incoming reactants called an "activated complex", which proceeds to drive the energy of the system over the required energy hump and to the lower energy state of the products of the reaction.
Reaction rates are ruled by the slow step in a chain of reaction transitions, and each transition can have its reaction rate sped up by the use of catalysts that participate but remain available in the system to mediate the next transition of an activated complex into products.
Interestingly, gas phase reactions ARE mostly reversible in the physical world, outside of the lab or the production facility at the chemical plant, where we coerce processes to move in certain productive and profitable directions.
This is why the search for life by telescopes of varying kinds is always a search for what the NASA scientists call the "water hole" which is now considered a necessary piece of evidence of extraterrestrial life in the universe.
Life Is Water and Water Is Life
It is in liquid phase and especially in hydrogen-bonding liquid water, where life gets its ability to reliably construct proteins, enzymes, lipids and nucleic acids by alternating transitions between the reversible and the irreversible. These transitions between the stability of entangled bonds and their decoherence and construction of new metastable entangled bonds until the activated complex is constructed and final catalysis (typically) drives the system over the energy hump irreversibly to the intended entangled products are what supports living systems. Everything and everyone around you does covalent chemistry, and they and you are utterly and minutely entangled systems.So, you never see messenger RNA spooling backwards out of a ribosome and turning protein into amino acids. Protein transcription only moves in the forward direction from amino acids transcribing messenger RNA at the ribosome like a tape reader and spooling off protein chains, entirely due to the reaction occurring in aqueous (watery) solution where there is a well-regulated and thoroughly cool enough environment to prevent local heating from undoing nature's work.
From Molecular Reaction Dynamics by Raphael D. Levine in the library, section 6.1.1 The Point of No Return and the Transition State, p. 203:So the answer to the question "What is life?" is in effect, water. It allows us to breath in oxygen and perform the biochemical functions of the cell in support of our moment to moment existence. Here are some detailed references on how breathing works: and knowing the details, you might want to stop smoking anything and get your Influenza shots and updated Covid boosters:
"Dealing with thermal reactants and with barriers that are high compared to thermal energies [at the temperature of the of cool water as the reaction medium] the assumption is quite reasonable that if the barrier has been crossed, the motion downhill will not reverse upon itself. At higher energies [like a hot gas or hot solid medium] when the barrier becomes less of a handicap, the barrier can be recrossed. But Transition State Theory is intended to be useful at ordinary temperatures [at an aqueous medium] when, due to the Boltzmann factor, there is not much excess energy for crossing the barrier."
- https://en.wikipedia.org/wiki/Respiration_(physiology))
- https://en.wikipedia.org/wiki/Pulmonary_alveolus
- https://en.wikipedia.org/wiki/Pulmonary_surfactant
- https://en.wikipedia.org/wiki/Respiratory_system#Gas_exchange
Shining A Light On Animate Matter Lowers Entropy Whereas Shining A Light On Inanimate Matter Raises Entropy
Like Professor Brian Greene and Professor Edward Witten, Professor Max Tegmark is a brilliant physicist and they all three are fans of the ascientific fantasy of string theory, and probably a few more of the ascientific fantasies on Sabine Hossenfelder's list (2/3 of the way down here.) Bless their hearts, but nevertheless they are each brilliant expositors of scientific physics and are really great to listen to. In this reasonably short video, Max Tegmark describes the quantum mechanical difference between living matter and non-living matter. [Stick with it through the Spekkens information theory statistical QM descriptions, he is talking to other QM theorists.]Max says that when photons "scan" through non-living matter the entropy increases. However, when photons "scan" through living matter, the entropy decreases. Living things respond to external stimuli and evolve, react and learn accordingly. Living things evolve by becoming more complex in a highly ordered and genetically remembered way, and the most ordered (lowest entropy) living organ (or frankly, system of any kind) is the nervous system and the brain. And the most complex and ordered system that we know of in the universe is the human brain, which is more like an analog switching system and not digital at all: there are no registers, just nerve cells interacting with the voltage differences created in axon/dendrite switching networks.
A fruit fly brain has 20 million synaptic connections, but a human brain has 100 trillion connections all firing and changing neural voltages even when we sleep. One could argue that makes for a lot of moving parts and higher entropy (s = kB ln Ω), however that brain has effectively one state (Ω=1) and that is your consciousness, and the natural log of one is zero: an astonishingly low entropy.
Also, there is no "small amount of arithmetic" because there is no integer or floating point unit, the brain emulates those digital systems in the gray matter with vastly slower performance than your typical calculator.
Hence we living systems with brains are capable of formal logic proving our theorems to be true according to Gödel's Completeness Theorem, whereas digital systems which use a "small amount of arithmetic" just to find each instruction address, memory register and virtual address are permanently restricted to following Gödel's Incompleteness Theorems I and II. So, we should stop worrying about the coming digital supremacy over humans, or any other living beings, for that matter. Computers cannot deduce with strong logic, they can only induce with weak logic. A robot can kill you, but a human programmer will have engineered your demise, either intentionally or by neglect. Robots will never be certain of the difference between what is right and what is wrong. We can have faith and make reasoned decisions based on it.
From The Man with the Golden Gun:
Bond: Moneypenny, you are better than a computer.
Moneypenny: In all sorts of ways! But, you never take advantage of them.
Seeing the Correct Path through the Fog of Reality and Ideality
When light enters the eye and interacts with the rods (black and white) and the cones (colors), the optic nerves stream those raw physical optical signals through the thalamus in the middle of your head and stream that into the visual cortex in the back of your head. In the visual cortex, raw signals become stereo vision with full colors, recognized shapes and objects, like the face of your parents and grandparents, etc., and that logical visual stream passes back through the thalamus with all the metadata tags on the recognized elements and then up to the cerebral cortex at the top of your head, where your world view is integrated with the other four senses whose signals have arrived ahead of vision due to less processing overhead (which is why foot races start with a gun and not a starting light.)Interestingly, there are six times as much processed logical visual signals flowing through the thalamus from the visual cortex as the original raw physical visual flow from the optic nerves. This explains why those people you see walking down the street having a conversation without a cell phone are really seeing someone they are talking to. Their echoes from the past are replaying from the visual cortex and appear as real as the raw optical flow, maybe even more real.
What I perceive when I chant to the Gohonzon arises entirely from inside me. What a digital system sees when it looks at the Gohonzon will not likely ever arise from inside, it will arise from code, once again, written by a human programmer, or generated by a machine programmed by a human programmer.
I give you Abraham Lincoln as proof of the permanent supremacy of living beings over the inanimate. He demonstrates the difference between (1) the imperfect expedient means employed by all the Buddhas to steadily improve the lives of living beings, and (2) the impractical and impossible perfection of thought, word and deed. No machine will ever get this right.
Describing Lincoln, historian Jon Meacham notes that there were three critical moments that reflected his principles while employing the expedient means of his Presidency, which always bent towards the direction of the Declaration of Independence as his personal compass:
- Immediately after his first election as President in February 1861, the Crittenden compromise, which was immensely popular even with his staff, was placed on the table by a Kentucky Senator to preserve slavery and extend it into some of the territories, to avoid war with the South. Lincoln said no. If slavery would be allowed to move into the territories, it would take root for decade upon decade, upon decade.
- The moment he enters office in March 1861, Fort Sumter is under siege. Secretary Seward, General Winfield Scott (Anaconda Plan) and others are not enthusiastic about fortifying Sumter. Lincoln said no. This is the point beyond which we will not concede, "and so the war came", as Lincoln said.
- In 1864, as Lincoln believes he will lose re-election, Lincoln is told by the Republican National Committee that if he keeps emancipation as a precondition for peace, he will lose and he needs to abandon this. In the middle of August in 1864, less than three months from the election, Lincoln said no. As he put it, "men act on incentive." How could he ask the black men under arms, who were defending the constitution of the United States to fight for anything other than their freedom? Then General Sherman takes Atlanta, the South is cut in half and Lincoln wins.
"Viewed from the genuine abolition ground, Mr. Lincoln seemed tardy, cold, dull, and indifferent; but measuring him by the sentiment of his country, a sentiment he was bound as a statesman to consult, he was swift, zealous, radical, and determined."That is the very definition of expedient means. It is nini funi (two but not two) with the true path: two in appearance, but one in essence.
Meacham goes on:Like the expedient means that he regularly employed, Lincoln is nini funi with the true Buddha: appearing an imperfect and indifferent agent of the Lotus Sutra, but in essence the Buddha of Beginningless Time. Because of his faith and dedication, he did not live to reach the nation's Centennial in 1876, falling 11 years short by assassination. However, after his death, or perhaps because of it: the 13th, 14th and 15th Amendments allowed the Union that he lived and died for to reach many of the milestones laid out in his personal compass of the Declaration of Independence.
"History is not a fairy tale. There can be light. There can be dark.
But the agents, and Lincoln understood this in the marrow of his bones, the human agents are imperfect.
And so if you're looking for a perfect embodiment of light, you should look to the church, look to the world of philosophy, look to the world of fiction, look to the world of legend, but we live in a political world.
We sit in a moment now where our divisions are as deep as they have been since the 1850s. we have competing visions of America that are not just about the mediation of differences.
We're not arguing about marginal tax rates, here, we're arguing about the very understanding of power and democracy and will politics be a mediation of differences or will it be total war."
With the same kind of faith that Lincoln had in the better angels of human nature, we will also navigate through the current river of storms to reach the 2030 Centennial of the SGI. Even if individually, some of us don't make it through to the promised land of 2030.
Of course, that would depend on the noblesse oblige of Bianca ProMAGA and the SGI Whisperers kindly allowing us to continue doing Kosen Rufu.
From Dr. No:
Bond: World domination. That same old dream. Our asylums are full of people who think they're Napoleon... or God.
2022.06.23 06:08 AnEvolvedPrimate Does computer animation give people false impressions of how cellular biology actually works?
Summary:
Computer animations of cellular biology often depict cells as machine-like and highly organized. ID advocates use this type of animation to sell the idea that cells are basically machines requiring intelligent design. Yet these depictions are highly misleading and actual cellular biology is far more chaotic and messy. Would more authentic depictions of cellular functions give people pause in thinking of cells as being highly organized, designed objects?
Discussion:
There is a fascinating thread on Peaceful Science about descriptions and depictions of cellular biology: Analogies to Motors
Building on that discussion, I'm curious as to the role that 3D animated movies about cellular biology have in terms of creating concepts or misconceptions about how that biology functions.
Take this video promo for Signature in the Cell: Signature in the Cell by Stephen Meyer (3:34 video)
It features slick, clean 3D animation depicting protein synthesis in a highly machine-like and organized fashion. This coupled with narration to reinforce the idea of machine-like processes and the messaging is quite effective. Reading through the comments on that video, lots of people are obviously wowed by it.
Yet the actual behavior inside cells is far more chaotic and random.
Per the following quote from Peter Moore's paper, How Should We Think About the Ribosome? (referenced in the above Peaceful Science thread):
If such a promo had to use a more realistic chaotic depiction of such processes, would people be as impressed? Would people still think of these cellular processes as being machine-like and requiring an intelligent designer?
For further reference (credit to the above Peaceful Science thread) is a video by Johannes Jaeger explaining that depictions of cells as machines is misleading and explaining alternative conceptualizations for cellular processes: The Cell Is Not a Machine – Beyond Networks: The Evolution of Living Systems (34:12 video)
The Jaeger video is based on this paper by Daniel Nicholson: Is the Cell Really a Machine?
submitted by AnEvolvedPrimate to DebateEvolution [link] [comments]
Computer animations of cellular biology often depict cells as machine-like and highly organized. ID advocates use this type of animation to sell the idea that cells are basically machines requiring intelligent design. Yet these depictions are highly misleading and actual cellular biology is far more chaotic and messy. Would more authentic depictions of cellular functions give people pause in thinking of cells as being highly organized, designed objects?
Discussion:
There is a fascinating thread on Peaceful Science about descriptions and depictions of cellular biology: Analogies to Motors
Building on that discussion, I'm curious as to the role that 3D animated movies about cellular biology have in terms of creating concepts or misconceptions about how that biology functions.
Take this video promo for Signature in the Cell: Signature in the Cell by Stephen Meyer (3:34 video)
It features slick, clean 3D animation depicting protein synthesis in a highly machine-like and organized fashion. This coupled with narration to reinforce the idea of machine-like processes and the messaging is quite effective. Reading through the comments on that video, lots of people are obviously wowed by it.
Yet the actual behavior inside cells is far more chaotic and random.
Per the following quote from Peter Moore's paper, How Should We Think About the Ribosome? (referenced in the above Peaceful Science thread):
It follows that if a movie of elongation is not to be totally misleading, it must depict the endless series of meaningless, thermally driven, conformational fluctuations that separate one functionally significant event from the next. However, even if it did so with perfect accuracy, it would still provide its viewers with far less useful information than a movie of a macroscopic machine would provide. A movie of a macroscopic machine can explain why the machine works because the motions of its components, which the movie displays, are all directly related to its function. By contrast, 99.99% of the motions portrayed in a realistic movie of elongation will be random fluctuations that have nothing to do with function.The aforementioned animation promo for Signature in the Cell doesn't depict anything of the kind. No wildly chaotic, random fluctuating movements. Just a slick, methodical, machine-like process.
If such a promo had to use a more realistic chaotic depiction of such processes, would people be as impressed? Would people still think of these cellular processes as being machine-like and requiring an intelligent designer?
For further reference (credit to the above Peaceful Science thread) is a video by Johannes Jaeger explaining that depictions of cells as machines is misleading and explaining alternative conceptualizations for cellular processes: The Cell Is Not a Machine – Beyond Networks: The Evolution of Living Systems (34:12 video)
The Jaeger video is based on this paper by Daniel Nicholson: Is the Cell Really a Machine?
2021.12.20 17:00 RectangularChocolate 211220 Weekly NCTeatime 🍵
Hello and welcome to this week's NCTeatime!
This is a free-for-all thread. Feel free to to drop a song/drama/movie recommendation, share a story, yell into the void, ask a question,etc.
Please remember to read the rules as well as the general Reddiquette. You can find our past NCTeatime/weekly discussion threads here.
Weekly Recap:
211213
211219
General reminders:
submitted by RectangularChocolate to NCT [link] [comments]
This is a free-for-all thread. Feel free to to drop a song/drama/movie recommendation, share a story, yell into the void, ask a question,etc.
Please remember to read the rules as well as the general Reddiquette. You can find our past NCTeatime/weekly discussion threads here.
Weekly Recap:
211213
- Check out the promotional poster for NCT 127 - Neo City: Seoul The Link
- NCT's third full length album, Universe, recorded 1,702,142 pre-orders as of December 13th! Congrats!
- Amazing! Awesome! And Beautiful! Listen to NCT's new song, Beautiful
- Vrooooom vroom... find where and how to listen to the rest of the album here
- Watch Jeno and Donghae behind the scenes of 'California Love'
- WayV became the first Chinese group to break the Melon top 100! Well deserved.
- Not one... not two... but twelve consecutive weeks on Billboard's 200 with a 2021 album... breaking records, NCT 127!
- Behind the scenes of Winwin and Ten's photoshoot with Madame Figaro
- Sweet moves! Check out NCT U's dance practice for Universe (Let's Play Ball) here
- Keep Growingz! EuMarkJungsim
- Awsaz special episode alert! Watch Yuta and Xiaojun on the latest episode of It's Awkward, But it's Okay
- Is it a bird? Is it a plane? No, it's [WayV-Log] Rock Climbing with Ten!
- Unbox the Universe (album) with NCT
- NCT 2021 - EuMarkJungsim Episode 3
- Watch the 8th episode of NCT 127's Analog Trip here
- NCT U's Universe (Let's Play Ball) at the 2021 KBS Song Festival
- Proteins, Ribosomes, and... NCT 127's 'Amino Acid' (OST for Analog Trip)
211219
General reminders:
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2021.09.24 04:17 Due-Bumblebee7805 10 scientific non-problems with biological and chemical evolution. part 2
Problem 2: Unguided Chemical Processes Cannot Explain the Origin of the Genetic Codeand we already have a problem. Abiogenesis did not happen purely by chance, it happened by specific chemical reactions. and if you don't know chemistry isn't random
Let’s assume, again, that a primordial sea filled with life’s building blocks did exist on the early Earth, and somehow it formed proteins and other complex organic molecules. Origin of life theorists believe that the next step in the origin of life is that — entirely by chance — more and more complex molecules formed until some began to self-replicate. From there, they believe Darwinian natural selection took over, favoring those molecules which were better able to make copies. Eventually, they assume, it became inevitable that these molecules would evolve complex machinery — like that used in today’s genetic code — to survive and reproduce.
Have modern theorists explained how this crucial bridge from inert nonliving chemicals to self-replicating molecular systems took place? The most prominent hypothesis for the origin of the first life is called the “RNA world.” In living cells, genetic information is carried by DNA, and most cellular functions are carried out by proteins. However, RNA is capable of both carrying genetic information and catalyzing some biochemical reactions. As a result, some theorists postulate the first life might have used RNA alone to fulfill all these functions.there are actually known ways for RNA to form on a prebiotic earth. for example, clay has been shown the be able to absorb and catalyze nucleotides, forming RNA https://sci-hub.se/https://doi.org/10.2113/gselements.1.3.145. here is a review article that goes into all of the research on origin of life, including the formation of RNA.
But there are many problems with this hypothesis.
For one, the first RNA molecules would have to arise by unguided, non-biological chemical processes. But RNA is not known to assemble without the help of a skilled laboratory chemist intelligently guiding the process. New York University chemist Robert Shapiro critiqued the efforts of those who tried to make RNA in the lab, stating: “The flaw is in the logic — that this experimental control by researchers in a modern laboratory could have been available on the early Earth.”15
Second, while RNA has been shown to perform many roles in the cell, there is no evidence that it could perform all the necessary cellular functions currently carried out by proteins.16this claim comes from Signature in the Cell: DNA and the Evidence for Intelligent Design, p. 304. the problem with Myers claim in the book is that he is comparing the needs of modern life to the first life, which would've been immensely more simple https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2926753/
Third, the RNA world hypothesis does not explain the origin of genetic information.but this does https://iubmb.onlinelibrary.wiley.com/doi/pdf/10.1002/iub.146
RNA world advocates suggest that if the first self-replicating life was based upon RNA, it would have required a molecule between 200 and 300 nucleotides in length.17 However, there are no known chemical or physical laws that dictate the order of those nucleotides.18 To explain the ordering of nucleotides in the first self-replicating RNA molecule, materialists must rely on sheer chance. But the odds of specifying, say, 250 nucleotides in an RNA molecule by chance is about 1 in 10150 — below the universal probability boundary, or events which are remotely possible to occur within the history of the universe.19 Shapiro puts the problem this way:the 200 and 300 nucleotide length comes from this article from nature https://www.nature.com/articles/35053176. here is the quote
The sudden appearance of a large self-copying molecule such as RNA was exceedingly improbable. … [The probability] is so vanishingly small that its happening even once anywhere in the visible universe would count as a piece of exceptional good luck.20
The class I ligase is an excellent starting point for attempts to evolve a replicase but does have one drawback. Its minimal catalytic domain is about 100 nucleotides long. When coupled to additional domains that may be required for proper template binding, fidelity and strand separation, the total length could approach 200–300 nucleotides. The longer the replicase, the more difficult the problem of replication, so shorter replicases should be looked for. One approach would be to use more highly activated nucleotide substrates, such as the phosphor-imidazolides. As these substrates are more reactive, less rate enhancement would be required to achieve extension rates in the range of one nucleotide per minute or per second, and a simpler and shorter ribozyme might suffice. Clearly, there are many possible approaches to evolving an RNA replicase, all of which bear investigation.as you can see, it's saying nothing of the sort. not only that but this article counters the whole rna is too complex argument https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3495036/
Fourth — and most fundamentally — the RNA world hypothesis does not explain the origin of the genetic code itself. In order to evolve into the DNA / protein-based life that exists today, the RNA world would need to evolve the ability to convert genetic information into proteins. However, this process of transcription and translation requires a large suite of proteins and molecular machines — which themselves are encoded by genetic information. This poses a chicken-and-egg problem, where essential enzymes and molecular machines are needed to perform the very task that constructs them.
The Chicken and the DVDhere is a paper explaining the evolution of protein synthesis https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3312679/
To appreciate this problem, consider the origin of the first DVD and DVD player. DVDs are rich in information, but without the machinery of a DVD player to read the disk, process its information, and convert it into a picture and sound, the disk would be useless. But what if the instructions for building the first DVD player were only found encoded on a DVD? You could never play the DVD to learn how to build a DVD player. So how did the first disk and DVD player system arise? The answer is obvious: a goal directed process — intelligent design — is required to produce both the player and the disk at the same time.
In living cells, information-carrying molecules (e.g. DNA or RNA) are like the DVD, and the cellular machinery which reads that information and converts it into proteins are like the DVD player. Just like the DVD analogy, genetic information can never be converted into proteins without the proper machinery. Yet in cells, the machines required for processing the genetic information in RNA or DNA are encoded by those same genetic molecules — they perform and direct the very task that builds them.
This system cannot exist unless both the genetic information and transcription / translation machinery are present at the same time, and unless both speak the same language. Biologist Frank Salisbury explained this problem in a paper in American Biology Teacher not long after the workings of the genetic code were first uncovered:
It’s nice to talk about replicating DNA molecules arising in a soupy sea, but in modern cells this replication requires the presence of suitable enzymes. … [T]he link between DNA and the enzyme is a highly complex one, involving RNA and an enzyme for its synthesis on a DNA template; ribosomes; enzymes to activate the amino acids; and transfer-RNA molecules. … How, in the absence of the final enzyme, could selection act upon DNA and all the mechanisms for replicating it? It’s as though everything must happen at once: the entire system must come into being as one unit, or it is worthless. There may well be ways out of this dilemma, but I don’t see them at the moment.21
Despite decades of work, origin-of-life theorists are still at a loss to explain how this system arose. In 2007, Harvard chemist George Whitesides was given the Priestley Medal, the highest award of the American Chemical Society. During his acceptance speech, he offered this stark analysis, reprinted in the respected journal, Chemical and Engineering News:
The Origin of Life. This problem is one of the big ones in science. It begins to place life, and us, in the universe. Most chemists believe, as do I, that life emerged spontaneously from mixtures of molecules in the prebiotic Earth. How? I have no idea.22
Similarly, the aforementioned article in Cell Biology International concludes: “New approaches to investigating the origin of the genetic code are required. The constraints of historical science are such that the origin of life may never be understood.”23 That is, they may never be understood unless scientists are willing to consider goal-directed scientific explanations like intelligent design.
But there is a much deeper problem with theories of chemical evolution, as well as biological evolution. This pertains not just to the ability to process genetic information via a genetic code, but the origin of that information itself.
conclusion: Luskin still has not present any problems for evolution or abiogenesis and dose not seem to actually look at the scientific lecture
original article https://www.discovery.org/a/24041/#fn16
2021.08.30 15:56 SteakhouseBlues Ten Problems (Repost)
Covinfo's Ten Problems with the Covid19 Vaccines (Updated for August 26th 2021)
The current Covid19 vaccines have 10 main problems:
0. First a Brief Explanation of How the New Covid19 Vaccines are Supposed to Work
There are two types vaccines, the moderna/Pfizer and the Johnson & Johnson/AstraZeneca. Both types use the same core principles to elicit an immune response. The MP type use a lipid nanoparticle and mRNA, whereas the J&JAZ type use an adenovirus and DNA. With the J&JAZ they took an existing virus, removed its normal genetic material and replaced it with a strand of modified DNA. They pump your body full of these adenovirus particles which infect your cells with the modified DNA. This DNA travels from the cytoplasm of your cell into the nucleus of your cell, which houses the rest of your cell's DNA. The modified DNA is then unzipped to produce two strands of mRNA. These messenger RNA strands carry a message, like a work order. They tell your cell what to build and where to put it. The mRNA strands leave the nucleus and are read by the ribosomes which translate the work order. It tells them to construct spike proteins and to anchor them on the membrane of the cell. Once those spike proteins are on the outside of your cells your body's immune cells, the macrophages come along and encounter them. They identify the spike proteins as foreign matter and kill your spike protein expressing cells. They gobble up and analyze the pieces of your newly killed cells and may call in other macrophages and dendritic cells for back up. Once the dendritic cells arrive, they will also destroy the spike expressing cells, believing them to be foreign invaders. They will analyze the pieces of your cells and take them to where the T-cells and B-cells are stored. They show all the parts of the dead cells (including the human parts) to these T- and B-cells, which will create antibodies that will attach to those parts. They're not supposed to create antibodies for your own parts, just for the S-protein. This way, when covid enters your body for real, the immune system already has antibodies to the spike protein and your body can move quickly to combat the virus. The moderna and Pfizer vaccines work in much the same way, except there are fewer steps. The MP vaxxes use lipid nanoparticles that are little bubbles of fat with a strand of mRNA in them. Once these nanoparticles are injected into the body, they get gobbled up by your cells and the nanoparticles release the mrna strands into the cytoplasm of your cell. Your ribosomes then read the mrna, just the same as with the J&JAZ vax and get to work producing spike proteins to display on the membrane of your cell. The rest is identical. (This is a very simplistic explanation of a very complex process, some steps have been skipped over and some processes have been simplified for the sake of brevity but the general gist of the process is accurate).
1. The Dangers of the Spike Protein
The spike protein of the virus, that is also being utilized in the vaccines, is damaging to our cells through 3 mechanisms. The first is that when the spike protein binds to the ACE2 receptor it causes the ACE2 to send signals to the mitochondria within the cell which destroys the mitochondria, eventually killing the cell. The second is that when the spike protein binds to our ACE2 receptors it causes the ACE2 to send signals to other cells which increases the amount of pro-inflammatory agents in the blood. This inflammation damages the tissues. The third way is that when the spike protein binds to the ACE2 of the platelets in our blood, it causes them to clot. Now, the vaccine manufacturers did take steps to make the spike protein more safe. The spike protein has two parts an S1 subunit and an S2 subunit. The S1 is the part that connects to the ACE2, and the S2 is the part that opens up like a knife stabbing the membrane and facilitates fusion between the membrane of the cell and the envelope of the virus. With the vaccines, they modified the S2 subunit so that it could not open up and jab into the cell membranes if it connects with any ACE2 receptors. They thought this would make the spike protein safe, but this assumption is false and if they had taken the time to do more research before rushing to production they would have found that out. It may seem like the jabby bit is what damages the cells, but actually the major damage is caused by the S1 connecting to the ACE2 receptor. Just the S1, by itself without the S2, causes the ACE2 receptor to start the cell signaling processes that cause the mitochondrial damage, the pro-inflammatory response, and the blood clots. OK, but the spike proteins are supposed to be anchored to the membranes of our cells, so how can they do all this damage if they remain planted on the outside of our cells? The spikes are supposed to stay anchored to our cell membranes, and on paper that should be what happens, but in practice they don't seem to remain anchored. There is evidence that in some people the spikes get dislodged and can end up circulating in our system. Once they are in circulation, they are free to connect with the ace2 receptors on our hearts, lungs, brains, etc, and are free to cause the aforementioned inflammation, blood clots, and cell death. Another issue is that the spikes can cause damage without ever being dislodged. The biodistribution data for Pfizer shows that a significant amount of it does make its way throughout the body. When the vaccine seeps into the bloodstream, the adenovirus/nanoparticles will encounter the walls of your veins. They will then transfect the DNA/mRNA into the endothelial cells that line the veins. These cells are supposed to be silky smooth to allow for efficient blood flow. Once the mRNA is read and the spike proteins are displayed on the surface of our endothelial cell membranes, those tubes will no longer be smooth. They'll have tiny little spike proteins sticking out of them. In big veins this will have little to no effect. But in the capillary networks where the tubes narrow considerably and the blood flow slows way down, these spikes will connect with the platelets in the blood. That will cause the blood clotting, even if the spikes themselves never get dislodged from the cell membranes. This will lead to millions of tiny blood clots in the capillaries, which will likely do little harm if they occur in a non-critical location or if they can be cleared out quickly enough (it takes 3 to 6 months to clear a clot). But if these clots occur in critical junctions or if constant boosters ensure that our bodies have ever larger numbers of clots to remove, then our bodies make be overwhelmed and suffer serious harm.
How the virus uses the spike protein to enter human cells: https://www.nature.com/articles/d41586-021-02039-y
Journal article with evidence that the spike protein by itself can damage cells by binding to ACE2, causing the cells mitochondria to lose their shape and break apart: https://www.ahajournals.org/doi/10.1161/CIRCRESAHA.121.318902
Article on how the Covid19 spike protein binds to the ACE2 receptor of our platelets to cause blood clots: https://jhoonline.biomedcentral.com/articles/10.1186/s13045-020-00954-7
Article explaining that blood clots from the spike protein interacting with our platelets are associated with both COVID-19 infection and vaccination: https://journals.plos.org/plosmedicine/article?id=10.1371/journal.pmed.1003648
Article explains that just the S1 subunit of the spike protein can cause platelets to clot: https://www.medrxiv.org/content/10.1101/2021.03.05.21252960v1
Article with evidence that spike proteins do end up circulating in the blood, when they're not supposed to, they're supposed to be anchored on the cell membranes: https://academic.oup.com/cid/advance-article/doi/10.1093/cid/ciab465/6279075
More evidence that spike proteins do not stay on the cell membranes but end up circulating in the blood. This study aims to explain the blood clots caused by the J&J and AstraZeneca adenovector vaccines, they claim that the DNA isn't properly spliced and the spike proteins end up in the blood causing thrombosis when the spikes attach to the ACE2 receptors of the endothelial cells: https://www.researchsquare.com/article/rs-558954/v1
Article on how the spike protein can cause neurodegeneration: https://www.sciencedirect.com/science/article/pii/S0006291X2100499X?via%3Dihub
Article on how the Covid19 spike protein crosses the blood-brain barrier: https://www.sciencedirect.com/science/article/pii/S096999612030406X?via%3Dihub
Japanese article on how the Pfizer vax is associated with brain hemorrhaging: https://joppp.biomedcentral.com/articles/10.1186/s40545-021-00326-7
Article on how AstraZeneca is associated with blood clots in the brain: https://www.nejm.org/doi/full/10.1056/NEJMoa2104840
Article on how the spike protein in vaccines can cause cell damage via cell signaling: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7827936/
Article that when the spike protein binds to the ACE2 receptor it causes the release of soluble IL-6R which acts as a extracellular signal which causes inflammation (see the first paper for evidence that the spike causes the release of IL-6R and see the second paper for an explanation of how soluble IL-6R causes pro-inflammatory transcellular signaling: https://pubmed.ncbi.nlm.nih.gov/33284859/ And https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3491447/
Another article that Spike protein from covid or the vaccine causes inflammation through cell signaling, this time there is evidence that the spike protein causes senescence (premature aging) signals in the cell which attracts leukocytes that cause inflammation of the cell: https://journals.asm.org/doi/10.1128/JVI.00794-21
Spike protein by itself causes cell damage by eliciting a pro-inflammatory response: https://www.nature.com/articles/s41375-021-01332-z
Vaccine causes heart inflammation if it seeps into the veins. They could help prevent this to some extent by following the standard practice of aspirating the needle (pulling back to see if they're injecting to a vein). But they're not following standard procedure: https://academic.oup.com/cid/advance-article/doi/10.1093/cid/ciab707/6353927
Pfizer animal testing document that was obtained by Dr. Byram Bridle through a FOI request to the Japanese government which shows the biodistribution of the lipid-nano particles throughout the bodies and organs of the test subjects. This is evidence that the lipid nanoparticles do not stay in the injection site, but instead travel all throughout the body (go to pg 16/23 for the charts showing biodistribution over the course of 48hrs): https://files.catbox.moe/0vwcmj.pdf
Addendum to the above link. This blog post provides easy to understand information (with pictures) on the make-up of the lipid nanoparticles used in the Covid19 vaccines. It shows that the pharmaceutical companies could have designed them to have targeting ligands on the outside, so that the nanoparticles would only transfect the muscle cells. But instead the vax was designed with PEG polymers on the outside, so that the immune system will not be able to pick them up and put them in the trash. The PEG is what Byram Bridle says is the reason the vaccine travels throughout the body and since it does not have targeting ligands, it can transfect any type of cell: https://www.cas.org/resource/blog/understanding-nanotechnology-covid-19-vaccines
Article explaining how they stabilized the S-protein in the vaccines to stop it from opening up. Unfortunately, it still leaves the S1 subunit intact, which is what causes the mitochondrial damage, blood clots, and inflammation by binding with the ACE2: https://cen.acs.org/pharmaceuticals/vaccines/tiny-tweak-behind-COVID-19/98/i38
2. Vaccine Enhanced Immune Escape
Vaccine enhanced immune escape occurs when a poorly designed or weak vaccine helps create new variants. This happens in the exact same way as antibiotic resistance and regular old evolution. In the case of evolution, if you want to make an organism stronger, you put it under evolutionarily unfavorable conditions. This way you kill all the weak examples of the organism and leave just the strong ones. If you want heat resistant bacteria, put a petri dish full of bacteria under moderately high heat to kill 99% of the bacteria. Save the 1% that were able to survive, allow them to grow, and repeat the process over and over again while turning up the heat a little each time. Do this until you have a population of bacteria that are all extremely heat resistant. The same process occurs with antibiotic resistance. When you only take half your meds, you kill 99% of the bacteria and leave only the 1% that were more resistant to the drugs. Before they were a small part of the population but you've changed the conditions of their environment, so that they have an advantage. You've killed all the normal bacteria that the mutant variants had to compete with so the antibiotic resistant bacteria are the only strain. So they surge in population to take over your body and now the antibiotics don't work very well either. The principles apply to viruses and vaccines. If you produce a vaccine that elicits a weak immune response, you are creating an unfavorable environment for the virus. You'll kill the weak 99%, and leave the 1% mutant virus particles that are not hindered by the vaccine's antibodies. Whereas before these mutants were only a tiny part of the population and would have been unlikely to gain significantly in population. Now the environment is in their favor and these mutant virus particles surge in number because they no longer have to compete with the other virus particles and your bodies defenses do not work against them. They are now highly likely to transmit to the next person, whereas before they would likely not have been able to leave the host in which the mutation occurred. The current covid vaccines are good at creating variants for three reasons. First, some vaccine manufacturers require two shots and now also boosters because the first shot produces a very weak immune response. Second, the vaccines are very leaky. Even after you have gotten a full immune response from both shots, you can still get and transmit the virus onto others. Well, which virus particles are likely to get passed on by a fully vaccinated person? Clearly they will be those virus particles that have the ability to multiply quickly while avoiding the antibodies produced by the vaccines. This will create very virulent and antibody resistant variants. Watch for these variants in the news as time goes on, we're already seeing things like Delta, Lambda, Epsilon, etc. As we implement boosters, they will start to come at faster and faster rates, and over time data scientists will start to see timed correlations between the implementation of mass boosters and the emergence of new strains. Third, the vaccines do seem to help reduce the severity of the disease when people are infected (although this may change as new variants emerge). Why would this be a concern? Well, because of the leakiness of the vaccines we just spoke about. If you have very low symptoms but you can still get and transmit the virus, then you won't even realize that you're sick and you'll be spreading the virus to even more people as an asymptomatic carrier. So, these vaccines will only increase transmission by creating more and more asymptomatic carriers (although this may not be a bad thing, if everyone in the world gets the virus and everyone is asymptomatic, then there's really no need to care about covid anymore. But this is an unrealistic idealization that is unlikely to occur, some people will still get sick and die or suffer long haul covid). One additional point to address here is the claim that the unvaccinated are causing the emergence of new vaccine resistant variants. Let me be clear, the unvaccinated absolutely have the ability to facilitate the creation of new variants. However, it would require a statistically enormous number of people to get the virus before they could produce a new variant by chance. This is because a mutant virus particle will only make up a small portion of the virus population inside a person's body. Therefore, it is highly unlikely that this particular particle will be able to spread to a new person. Whereas, in the vaccinated, their weak immune response specifically selects for the mutant variants. It is highly likely that if a vaccinated person passes on the virus to another person, the particles they pass on will be those that have the ability to escape from the immune response elicited by the vaccines. An analogy would be if you did an experiment with 500 room temperature petri dishes filled with bacteria and 500 heated petri dishes with bacteria, then found a heat resistant variant but didn't know which dish it came from. It would be absurd to think that the heat resistant strain of bacteria came from the room temperature petri dishes. It would possible, sure, but completely improbable that the heat resistant strain had suddenly appeared in a room temp petri dish. There would be no reason for it to become a dominant strain in that environment. Logically, statistically, and evolutionarily, it must have come from the heated petri dishes. This is a very basic and obvious conclusion, but the media and government bureaucrats in lab coats are trying to tell you that the absurd thing is true. They're trying to say that the unvaccinated (the room temperature petri dishes) are where the vaccine resistant strains are coming from.
Geert Vanden Bossche is a virologist who has been sounding the alarm on this issue, you can visit his website or see a full collection of his videos down below: https://www.geertvandenbossche.org/
Evidence of cov2 immune escape: https://science.sciencemag.org/content/early/2021/06/30/science.abi7994
Article from 2015 that explains how imperfect vaccination (like the Pfizer and moderna that require at least two shots to be effective) can create immune escape variants: https://journals.plos.org/plosbiology/article?id=10.1371/journal.pbio.1002198
Article from 2021 explains that unless vaccination is done quickly, there will be a high probability of escape mutants: https://www.nature.com/articles/s41598-021-95025-3
CDC warns COVID-19 may be a few mutations away from evading vaccines. The virus isn't mutating to avoid the vaccines because of unvaccinated people, it's because the vaccines are putting evolutionary pressure on the virus: https://nypost.com/2021/07/27/cdc-covid-19-may-be-a-few-mutations-away-from-evading-vaccines/
3. Antibody Dependent Enhancement
There is a potential for ADE, antibody dependent enhancement. This is when the virus mutates so that the antibodies no longer neutralize the virus but the antibodies still try to attach to it. This can actually help the virus get into your immune cells because when the virus is covered with antibodies it will draw macrophages to the virus that will try to eat it. However, when your macrophages come to eat the virus particle that they think has been neutralized, the virus gets inside them and starts replicating because the antibodies actually didn't neutralize the virus. Your own antibodies act like a kind of Trojan Horse. Another way that ADE can happen is your own antibodies connect to the receptors of your cells and actually help the virus get in directly. This was a huge problem with the Dengue vaccine and we need to do a lot of testing to make sure this isn't a possibility. Clearly with these rushed vaccines we haven't eliminated this possibility and with the virus mutating, ADE may pop up with a later variant. We must stay vigilant and keep an eye out for this signal. It will manifest as people with high antibody levels being more likely to get sick and die.
Journal article from 2005 shows evidence that sars-cov1 vaccine, that also focused on the spike protein, caused ADE when subjects were challenged with different strain: https://www.nature.com/articles/news050110-3#ref-CR1
Article explaining how ADE works in Sar-cov1: https://www.nature.com/articles/s41586-020-2538-8
Article explaining the potential for ADE in Covid19: https://www.nature.com/articles/s41586-020-2538-8
Another article that speculates on the potential for ADE in Covid19: https://pubmed.ncbi.nlm.nih.gov/32920233/
Article explaining the potential risks of ADE in Sar-cov2: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7943455/
Article from 2021 explains that there is evidence that covid19 is able to kill macrophages by using antibody dependent mechanisms: https://www.biorxiv.org/content/10.1101/2021.02.22.432407v1
Paper explains that the delta variant is extremely close to developing the ADE, only a few mutations will allow it to use our own antibodies to enter our cells: https://www.biorxiv.org/content/10.1101/2021.08.22.457114v1
4. The Potential for Autoimmune Disorders
There is a potential for an autoimmune response from the vaccines. The vaccines that were developed for Sars-Cov-1 used the spike protein, just like the vaccines for Sars-Cov-2. Unfortunately, the old vaccines caused the animals to develop serious autoimmune disorders and causing severe organ damage. There is a question about whether these new vaccines, which also focus on the spike protein, will also cause autoimmune disorders. Since both the old vaccines and the new vaccines utilize the spike protein to elicit an immune response, there is a danger that the new vaccines will have the same issues. The problem is that autoimmune disorders take a long time to develop and to be detectable. It may take a long time before doctors and scientists can link the sudden rise in certain kinds of autoimmune disorders with these vaccines. Usually, in a vaccine trial you closely monitor your trial group for years and years. This allows you to identify the signals. With the current program of injecting millions of people, there will be no clear way to link causation to the vaccines and an increase in autoimmune disorders may just fly under the radar. We may not know for a very long time or we may never know. Another concern is that because of the way the mRNA vaccines work, they cause your own cells to present as foreign entities. Your immune system comes over and starts killing your own cells. This has never been done before in human history. We have no idea if there will be long term consequences for teaching your immune system to treat its own cells as foreign material. We will have to wait and see whether this will lead to autoimmune disorders. This means that caution, at the very least, is justified and rational.
Journal article from 2004 on autoimmune disorders from Sars-cov1 vaccine that also focused on the spike protein: https://www.cidrap.umn.edu/news-perspective/2004/12/sars-vaccine-linked-liver-damage-ferret-study
Journal article from 2005 on autoimmune disorders from Sars-cov1 vaccine that also focused on the spike protein: https://pubmed.ncbi.nlm.nih.gov/15755610/
Journal article from 2012 on autoimmune disorders from Sars-cov1 vaccine that also focused on the spike protein: https://journals.plos.org/plosone/article?id=10.1371/journal.pone.0035421
Journal article from 2020 on autoimmune disorders from Sars-cov vaccine (can't figure out if they're talking about cov1 or 2): https://jvi.asm.org/content/78/22/12672.abstract
Journal article from 2020 explains why immune disorders happen with covid vax, because human and Covid19 proteins are similar: https://www.sciencedirect.com/science/article/pii/S2589909020300186
5. The Narrow Design Focus of the Vaccines and Lack of Efficacy
The mRNA vaccines are narrowly focused on just the spike protein when they could have been designed to target more proteins. The Covid19 coronavirus has 4 main proteins. There are 3 on its outside and 1 on the inside. The S-protein, the M-protein, and the E-protein, are on the outside, while the N-protein is on the inside. When you get a natural infection your body will likely produce antibodies for all or most of these proteins (depending on the function of your own unique immune system). We knew from studying Sars-Cov-1 that antibodies to the S-protein and the M-protein are both neutralizing. In fact, they used exactly that knowledge when they designed the current vaccines. So, they could have tried to make vaccines that utilize the M-protein to avoid the potential for autoimmune disorders discussed above. But they didn't, they instead focused only on the S-protein. They could have designed the vaccines so that they present both the S-protein and the M-protein. This would have made the vaccines much more effective and less leaky since any mutated virus particles would have to have mutated both the S-protein and the M-protein to avoid the antibodies. Whereas, the current vaccines are narrowly focused on just the S-protein, meaning that the virus only has to mutate the one protein. It is exponentially harder for an organism to mutate two beneficial traits vs just mutating one beneficial trait. So, these vaccines are worse than they could have been. We are seeing the results of these mediocre medications in the data coming from highly vaccinated countries.
Article explains how vaccine manufacturers have used relative risk reduction to determine that vaccine efficacy is ~90+%, however they should have used absolute risk reduction which would tell us that the vaccines will only reduce total covid cases by ~1%: https://www.thelancet.com/journals/lanmic/article/PIIS2666-5247(21)00069-0/fulltext
Addendum to the above information. This video from 2013 explains the difference between relative and absolute risk reduction in a very simple way: https://www.youtube.com/watch?v=7K30MGvOs5s&ab_channel=TerryShaneyfelt
Article from 2005 explains that antibodies to the S-protein and the M-protein are effective in neutralizing the sars-cov1 virus. However, the sars-cov2 vaccines only target the S-protein. This is evidence that the vaccine manufacturers could have chosen to make a superior mrna vax that produced two types of antibodies, but chose to focus narrowly on just the S-protein: https://pubmed.ncbi.nlm.nih.gov/16544518/
Antibodies from vaccines start to drop within 6 months, get ready for endless boosters: https://www.nature.com/articles/s41586-021-03777-9
Iceland covid data shows majority of covid cases are fully vaccinated: https://www.covid.is/data
UK data for August 2021 shows 183,000 unvaccinated cases with 390 deaths, and 73,000 vaccinated cases but with 679 deaths. So, it seems that getting vaccinated reduces your chances of getting covid, but increases your chances of dying from it if you do get it: https://assets.publishing.service.gov.uk/government/uploads/system/uploads/attachment_data/file/1012644/Technical_Briefing_21.pdf
Vaccinated healthcare works who experienced a vaccine failure still had huge viral loads: https://papers.ssrn.com/sol3/papers.cfm?abstract_id=3897733
Pfizer intentionally destroyed the control groups in their trials for the covid vaccine, which means we'll never know how effective the vaccine actually is: https://www.npr.org/sections/health-shots/2021/02/19/969143015/long-term-studies-of-covid-19-vaccines-hurt-by-placebo-recipients-getting-immuni
Moderna has never been able to get a drug or vaccine approved by the FDA, they were chosen by Trump because the CEO said they could get their experimental gene therapy vaccine made in the fastest time, no animal trials were done: https://www.cnn.com/2020/05/01/us/coronavirus-moderna-vaccine-invs/index.html
Moderna CEO Stephane Bancel explains that they designed the vaccine in just two days: https://v.redd.it/p83r1m7zzgd71
Even CNN agrees the rushed vaccine is a stupid idea (but only while Trump was president): https://edition.cnn.com/2020/09/01/health/eua-coronavirus-vaccine-history/index.html
6. There are Alternatives to Vaccination
There are alternative treatments that are effective against Covid19 but they are being suppressed. Why? Because the vaccines are not approved by the FDA but instead they are emergency use authorized only. The emergency use authorization can only be granted if "there are no adequate, approved, and available alternatives". Well, a growing body of scientific research is showing that both Ivermectin and Fluvoxamine (among other drugs) are adequate alternatives for early treatment of Covid19, and both of these drugs have been FDA approved for years. Unfortunately, that means they are now off patent and no one can make any money off of them. So, for the vaccines to continue to receive their EUA, the existence of these treatments must be suppressed. We have seen a huge amount of censorship of doctors who have been speaking out about these drugs.
Ivermectin
Emergency use authorization for the vaccines cannot be granted if there are effective alternative approved treatments for Covid19. So, if the pharmaceutical industry is going to make any money off covid, they must suppress the existence of any existing off patent drugs that may be effective in treating or preventing covid: https://www.fda.gov/emergency-preparedness-and-response/mcm-legal-regulatory-and-policy-framework/emergency-use-authorization
Meta-analysis on the efficacy of Ivermectin in treating Covid19: https://journals.lww.com/americantherapeutics/Abstract/9000/Ivermectin_for_Prevention_and_Treatment_of.98040.aspx
A double-blind, randomized placebo-controlled trial shows that Ivermectin is able to significantly reduce viral load within 6 days for most people: https://www.medrxiv.org/content/10.1101/2021.05.31.21258081v1
More evidence that Ivermectin treatment leads to much faster recovery from Covid19: https://onlinelibrary.wiley.com/doi/10.1002/jmv.26880
A study reveals that a five-day course of ivermectin for the treatment of COVID-19 may reduce the duration of illness: https://pubmed.ncbi.nlm.nih.gov/33278625/
Ivermectin stops replication of covid: https://www.sciencedirect.com/science/article/pii/S0166354220302011
Ivermectin has anti-viral properties: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3888155/
Ivermectin has anti-viral properties against covid: https://www.nature.com/articles/s41429-020-0336-
Ivermectin binds to Covid19 proteins to block the virus: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7996102/
Evidence that Ivermectin can be effective as a prophylaxis, Argentinian frontline healthcare workers were given Ivermectin as a preventative and zero got sick with covid, whereas 58.2% of the control group who did not take Ivermectin got covid: https://www.buongiornosuedtirol.it/wp-content/uploads/2021/04/Nota-Journal-of-Biomedical-Research-Safety-and-Efficacy-Iota-Carrageenan-and-Ivermectin.pdf
Ivermectin safe to give 12mg per day for 5 days: https://www.ijidonline.com/article/S1201-9712%2820%2932506-6/fulltext
Ivermectin safely administered 60mg per day for 6 months: https://www.tandfonline.com/doi/full/10.1080/10428194.2020.1786559
Fluvoxamine
Fluvoxamine helps in covid treatment: https://pubmed.ncbi.nlm.nih.gov/33180097/
Covid leads to long term inflammation, useful for long haul Covid19 treatment: https://pubmed.ncbi.nlm.nih.gov/33391730/
Fluvoxamine has anti-inflammatory properties that can help treat covid: https://www.frontiersin.org/articles/10.3389/fphar.2021.652688/full
Fluvoxamine targets sigma-1 to stop covid replication: https://pubmed.ncbi.nlm.nih.gov/33403480/
7. They are Pushing the Vaccine on People Who Clearly Don't Need It
We've known for decades that once you are infected with a virus or disease, your body creates a robust immune response, including memory T cells and B cells. These cells stick around so that you can quickly respond to a new infection. However, this fact is being completely ignored by vaccine pushers. They want a needle in every arm, even in the arms of those who do not need it, like the covid recovered. We might say, well covid is new and different, and perhaps immunity wanes after a time. This assumption was prudent in the beginning of the pandemic but now we have lots of evidence that the covid recovered have a near zero chance of getting sick again. Your body takes a few weeks and months to build up its antibodies after an infection. During this time your body is susceptible to a second infection. Most of the time when a second infection takes place, it occurs during this time of antibody build-up. There is no reason to force every covid recovered patient to take an invasive experimental drug, especially after that initial 3 month period after they have built up a sufficient immune response. If you still think that the miniscule chance that their immune system has failed makes them a danger, then why are these people not asked for proof of antibodies? It's because they don't actually care if you have antibodies. The vaccinated, without knowing whether they have antibodies or not, can walk around freely touching vegetables and sharing drinks, but a covid recovered patient, with proof of antibodies is still considered a biohazard. This is backass wards and it is evidence that vax pushers don't actually care about immunity. It is just about getting a needle into every arm. The reason why they are doing this, I do not know. I leave it up to you to speculate. But it doesn't make sense and I make a point of not going along with things that don't make sense.
No benefit from vaccination for previously infected individuals: https://www.medrxiv.org/content/10.1101/2021.06.01.21258176v2
Covid19 infection produces long lasting immunity: https://www.nature.com/articles/s41586-021-03647-4
Second article that covid19 infection produces life long immunity: https://www.nature.com/articles/d41586-021-01442-9
More evidence that covid19 infection produces long term immunity: https://www.medrxiv.org/content/10.1101/2021.04.19.21255739v1
Study of 600,000 covid recovered patients finds less than 1% reinfection rate over 10 months and an almost 0% risk in the first 7 months: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8209951/pdf/RMV-9999-e2260.pdf
8. The Growing Evidence of Adverse Reactions to the Vaccines and the Censorship of this Evidence
There is a growing amount of data that people are having severe reactions to the vaccines. It gets little to no coverage in the press, in some cases people who talk about their reactions on social media are being censored and called anti-vaxxers (I mean, how asinine to call someone who took the jab an anti-vaxxer) or fakers (I am sure some are faking for money/attention, but I highly doubt it's many of them given the social consequences for lying). Some senators have done press conferences with these vaccine harmed people so they can tell their stories. Some doctors have spoke out, although many are being censored and threatened with losing their licenses. Some internet platforms are still allowing people to tell their stories. But many communities are being deleted or shutdown. I remember when journalists, data scientists, and doctors were sounding the alarm on covid in January 2020 while all the authorites and big shot scientists were saying "no, no, everything is fine, it's just the flu bro, go hug a Chinese person, or are you a racist". What if those people had been censored then? Many of the same people who alerted us to covid are sounding the alarm on these vaccines now. We were lucky then that they were not censored. We are lucky now that there are publicly accessible government databases which contain reports of people who have had adverse reactions to the vaccines. These systems were put in place in the 90's to act as an early warning system and to give transparency to the public after previous botched vaccine rollouts, like the 1976 swine flu vaccine debacle. You can go and read these reports of adverse reactions to the vaccines for yourself. There are websites that download the reports and present them to the public in a very readable manner (the government website from the 90's is not very good). There are concerns that these reports are being made in error or by bad actors. However, research has been done into these systems and it was found that 86% of the adverse reactions had seemingly no other cause or explanation aside from the covid vaccine. In the past, if a vaccine hit 50 deaths or a few hundred adverse reactions on these reporting systems, they would shutdown the vaccination program. As of writing this, for the covid vaccines, the deaths in the US are above ten thousand and the serious adverse reactions are into the hundreds of thousands. Yet they just keep rolling with the shots and are even forcibly mandating them.
Analysis on the VAERS death data shows that in 86% of reports the vaccine cannot be ruled out as a causal factor in the death of the patient: https://www.researchgate.net/publication/352837543_Analysis_of_COVID-19_vaccine_death_reports_from_the_Vaccine_Adverse_Events_Reporting_System_VAERS_Database_Interim_Results_and_Analysis
Addendum to the above link. OpenVAERS is a site that allows you to easily read VAERS reports and breaks down the numbers. The reports seem to be a lot of people who have comorbidities or are old, but there are also some really eye opening cases where young people experience horrible side effects. Read for yourself and make up your own mind about what the vax is doing to your fellow Americans: https://www.openvaers.com/openvaers
9 & 10 Continued in the Comments
submitted by SteakhouseBlues to u/SteakhouseBlues [link] [comments]
The current Covid19 vaccines have 10 main problems:
- The spike protein is cytotoxic.
- The emergence of immune escape variants.
- The potential for antibody dependent enhancement.
- The potential for autoimmune disorders.
- The narrow design focus of the vaccines.
- There are alternative treatments to both prevent and treat covid.
- They are trying to jab everyone, even people who don't need it.
- There are serious adverse reactions to the vaccines.
- There is no liability for vaccine producers.
- There is potential for long term unknown side effects.
0. First a Brief Explanation of How the New Covid19 Vaccines are Supposed to Work
There are two types vaccines, the moderna/Pfizer and the Johnson & Johnson/AstraZeneca. Both types use the same core principles to elicit an immune response. The MP type use a lipid nanoparticle and mRNA, whereas the J&JAZ type use an adenovirus and DNA. With the J&JAZ they took an existing virus, removed its normal genetic material and replaced it with a strand of modified DNA. They pump your body full of these adenovirus particles which infect your cells with the modified DNA. This DNA travels from the cytoplasm of your cell into the nucleus of your cell, which houses the rest of your cell's DNA. The modified DNA is then unzipped to produce two strands of mRNA. These messenger RNA strands carry a message, like a work order. They tell your cell what to build and where to put it. The mRNA strands leave the nucleus and are read by the ribosomes which translate the work order. It tells them to construct spike proteins and to anchor them on the membrane of the cell. Once those spike proteins are on the outside of your cells your body's immune cells, the macrophages come along and encounter them. They identify the spike proteins as foreign matter and kill your spike protein expressing cells. They gobble up and analyze the pieces of your newly killed cells and may call in other macrophages and dendritic cells for back up. Once the dendritic cells arrive, they will also destroy the spike expressing cells, believing them to be foreign invaders. They will analyze the pieces of your cells and take them to where the T-cells and B-cells are stored. They show all the parts of the dead cells (including the human parts) to these T- and B-cells, which will create antibodies that will attach to those parts. They're not supposed to create antibodies for your own parts, just for the S-protein. This way, when covid enters your body for real, the immune system already has antibodies to the spike protein and your body can move quickly to combat the virus. The moderna and Pfizer vaccines work in much the same way, except there are fewer steps. The MP vaxxes use lipid nanoparticles that are little bubbles of fat with a strand of mRNA in them. Once these nanoparticles are injected into the body, they get gobbled up by your cells and the nanoparticles release the mrna strands into the cytoplasm of your cell. Your ribosomes then read the mrna, just the same as with the J&JAZ vax and get to work producing spike proteins to display on the membrane of your cell. The rest is identical. (This is a very simplistic explanation of a very complex process, some steps have been skipped over and some processes have been simplified for the sake of brevity but the general gist of the process is accurate).
1. The Dangers of the Spike Protein
The spike protein of the virus, that is also being utilized in the vaccines, is damaging to our cells through 3 mechanisms. The first is that when the spike protein binds to the ACE2 receptor it causes the ACE2 to send signals to the mitochondria within the cell which destroys the mitochondria, eventually killing the cell. The second is that when the spike protein binds to our ACE2 receptors it causes the ACE2 to send signals to other cells which increases the amount of pro-inflammatory agents in the blood. This inflammation damages the tissues. The third way is that when the spike protein binds to the ACE2 of the platelets in our blood, it causes them to clot. Now, the vaccine manufacturers did take steps to make the spike protein more safe. The spike protein has two parts an S1 subunit and an S2 subunit. The S1 is the part that connects to the ACE2, and the S2 is the part that opens up like a knife stabbing the membrane and facilitates fusion between the membrane of the cell and the envelope of the virus. With the vaccines, they modified the S2 subunit so that it could not open up and jab into the cell membranes if it connects with any ACE2 receptors. They thought this would make the spike protein safe, but this assumption is false and if they had taken the time to do more research before rushing to production they would have found that out. It may seem like the jabby bit is what damages the cells, but actually the major damage is caused by the S1 connecting to the ACE2 receptor. Just the S1, by itself without the S2, causes the ACE2 receptor to start the cell signaling processes that cause the mitochondrial damage, the pro-inflammatory response, and the blood clots. OK, but the spike proteins are supposed to be anchored to the membranes of our cells, so how can they do all this damage if they remain planted on the outside of our cells? The spikes are supposed to stay anchored to our cell membranes, and on paper that should be what happens, but in practice they don't seem to remain anchored. There is evidence that in some people the spikes get dislodged and can end up circulating in our system. Once they are in circulation, they are free to connect with the ace2 receptors on our hearts, lungs, brains, etc, and are free to cause the aforementioned inflammation, blood clots, and cell death. Another issue is that the spikes can cause damage without ever being dislodged. The biodistribution data for Pfizer shows that a significant amount of it does make its way throughout the body. When the vaccine seeps into the bloodstream, the adenovirus/nanoparticles will encounter the walls of your veins. They will then transfect the DNA/mRNA into the endothelial cells that line the veins. These cells are supposed to be silky smooth to allow for efficient blood flow. Once the mRNA is read and the spike proteins are displayed on the surface of our endothelial cell membranes, those tubes will no longer be smooth. They'll have tiny little spike proteins sticking out of them. In big veins this will have little to no effect. But in the capillary networks where the tubes narrow considerably and the blood flow slows way down, these spikes will connect with the platelets in the blood. That will cause the blood clotting, even if the spikes themselves never get dislodged from the cell membranes. This will lead to millions of tiny blood clots in the capillaries, which will likely do little harm if they occur in a non-critical location or if they can be cleared out quickly enough (it takes 3 to 6 months to clear a clot). But if these clots occur in critical junctions or if constant boosters ensure that our bodies have ever larger numbers of clots to remove, then our bodies make be overwhelmed and suffer serious harm.
How the virus uses the spike protein to enter human cells: https://www.nature.com/articles/d41586-021-02039-y
Journal article with evidence that the spike protein by itself can damage cells by binding to ACE2, causing the cells mitochondria to lose their shape and break apart: https://www.ahajournals.org/doi/10.1161/CIRCRESAHA.121.318902
Article on how the Covid19 spike protein binds to the ACE2 receptor of our platelets to cause blood clots: https://jhoonline.biomedcentral.com/articles/10.1186/s13045-020-00954-7
Article explaining that blood clots from the spike protein interacting with our platelets are associated with both COVID-19 infection and vaccination: https://journals.plos.org/plosmedicine/article?id=10.1371/journal.pmed.1003648
Article explains that just the S1 subunit of the spike protein can cause platelets to clot: https://www.medrxiv.org/content/10.1101/2021.03.05.21252960v1
Article with evidence that spike proteins do end up circulating in the blood, when they're not supposed to, they're supposed to be anchored on the cell membranes: https://academic.oup.com/cid/advance-article/doi/10.1093/cid/ciab465/6279075
More evidence that spike proteins do not stay on the cell membranes but end up circulating in the blood. This study aims to explain the blood clots caused by the J&J and AstraZeneca adenovector vaccines, they claim that the DNA isn't properly spliced and the spike proteins end up in the blood causing thrombosis when the spikes attach to the ACE2 receptors of the endothelial cells: https://www.researchsquare.com/article/rs-558954/v1
Article on how the spike protein can cause neurodegeneration: https://www.sciencedirect.com/science/article/pii/S0006291X2100499X?via%3Dihub
Article on how the Covid19 spike protein crosses the blood-brain barrier: https://www.sciencedirect.com/science/article/pii/S096999612030406X?via%3Dihub
Japanese article on how the Pfizer vax is associated with brain hemorrhaging: https://joppp.biomedcentral.com/articles/10.1186/s40545-021-00326-7
Article on how AstraZeneca is associated with blood clots in the brain: https://www.nejm.org/doi/full/10.1056/NEJMoa2104840
Article on how the spike protein in vaccines can cause cell damage via cell signaling: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7827936/
Article that when the spike protein binds to the ACE2 receptor it causes the release of soluble IL-6R which acts as a extracellular signal which causes inflammation (see the first paper for evidence that the spike causes the release of IL-6R and see the second paper for an explanation of how soluble IL-6R causes pro-inflammatory transcellular signaling: https://pubmed.ncbi.nlm.nih.gov/33284859/ And https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3491447/
Another article that Spike protein from covid or the vaccine causes inflammation through cell signaling, this time there is evidence that the spike protein causes senescence (premature aging) signals in the cell which attracts leukocytes that cause inflammation of the cell: https://journals.asm.org/doi/10.1128/JVI.00794-21
Spike protein by itself causes cell damage by eliciting a pro-inflammatory response: https://www.nature.com/articles/s41375-021-01332-z
Vaccine causes heart inflammation if it seeps into the veins. They could help prevent this to some extent by following the standard practice of aspirating the needle (pulling back to see if they're injecting to a vein). But they're not following standard procedure: https://academic.oup.com/cid/advance-article/doi/10.1093/cid/ciab707/6353927
Pfizer animal testing document that was obtained by Dr. Byram Bridle through a FOI request to the Japanese government which shows the biodistribution of the lipid-nano particles throughout the bodies and organs of the test subjects. This is evidence that the lipid nanoparticles do not stay in the injection site, but instead travel all throughout the body (go to pg 16/23 for the charts showing biodistribution over the course of 48hrs): https://files.catbox.moe/0vwcmj.pdf
Addendum to the above link. This blog post provides easy to understand information (with pictures) on the make-up of the lipid nanoparticles used in the Covid19 vaccines. It shows that the pharmaceutical companies could have designed them to have targeting ligands on the outside, so that the nanoparticles would only transfect the muscle cells. But instead the vax was designed with PEG polymers on the outside, so that the immune system will not be able to pick them up and put them in the trash. The PEG is what Byram Bridle says is the reason the vaccine travels throughout the body and since it does not have targeting ligands, it can transfect any type of cell: https://www.cas.org/resource/blog/understanding-nanotechnology-covid-19-vaccines
Article explaining how they stabilized the S-protein in the vaccines to stop it from opening up. Unfortunately, it still leaves the S1 subunit intact, which is what causes the mitochondrial damage, blood clots, and inflammation by binding with the ACE2: https://cen.acs.org/pharmaceuticals/vaccines/tiny-tweak-behind-COVID-19/98/i38
2. Vaccine Enhanced Immune Escape
Vaccine enhanced immune escape occurs when a poorly designed or weak vaccine helps create new variants. This happens in the exact same way as antibiotic resistance and regular old evolution. In the case of evolution, if you want to make an organism stronger, you put it under evolutionarily unfavorable conditions. This way you kill all the weak examples of the organism and leave just the strong ones. If you want heat resistant bacteria, put a petri dish full of bacteria under moderately high heat to kill 99% of the bacteria. Save the 1% that were able to survive, allow them to grow, and repeat the process over and over again while turning up the heat a little each time. Do this until you have a population of bacteria that are all extremely heat resistant. The same process occurs with antibiotic resistance. When you only take half your meds, you kill 99% of the bacteria and leave only the 1% that were more resistant to the drugs. Before they were a small part of the population but you've changed the conditions of their environment, so that they have an advantage. You've killed all the normal bacteria that the mutant variants had to compete with so the antibiotic resistant bacteria are the only strain. So they surge in population to take over your body and now the antibiotics don't work very well either. The principles apply to viruses and vaccines. If you produce a vaccine that elicits a weak immune response, you are creating an unfavorable environment for the virus. You'll kill the weak 99%, and leave the 1% mutant virus particles that are not hindered by the vaccine's antibodies. Whereas before these mutants were only a tiny part of the population and would have been unlikely to gain significantly in population. Now the environment is in their favor and these mutant virus particles surge in number because they no longer have to compete with the other virus particles and your bodies defenses do not work against them. They are now highly likely to transmit to the next person, whereas before they would likely not have been able to leave the host in which the mutation occurred. The current covid vaccines are good at creating variants for three reasons. First, some vaccine manufacturers require two shots and now also boosters because the first shot produces a very weak immune response. Second, the vaccines are very leaky. Even after you have gotten a full immune response from both shots, you can still get and transmit the virus onto others. Well, which virus particles are likely to get passed on by a fully vaccinated person? Clearly they will be those virus particles that have the ability to multiply quickly while avoiding the antibodies produced by the vaccines. This will create very virulent and antibody resistant variants. Watch for these variants in the news as time goes on, we're already seeing things like Delta, Lambda, Epsilon, etc. As we implement boosters, they will start to come at faster and faster rates, and over time data scientists will start to see timed correlations between the implementation of mass boosters and the emergence of new strains. Third, the vaccines do seem to help reduce the severity of the disease when people are infected (although this may change as new variants emerge). Why would this be a concern? Well, because of the leakiness of the vaccines we just spoke about. If you have very low symptoms but you can still get and transmit the virus, then you won't even realize that you're sick and you'll be spreading the virus to even more people as an asymptomatic carrier. So, these vaccines will only increase transmission by creating more and more asymptomatic carriers (although this may not be a bad thing, if everyone in the world gets the virus and everyone is asymptomatic, then there's really no need to care about covid anymore. But this is an unrealistic idealization that is unlikely to occur, some people will still get sick and die or suffer long haul covid). One additional point to address here is the claim that the unvaccinated are causing the emergence of new vaccine resistant variants. Let me be clear, the unvaccinated absolutely have the ability to facilitate the creation of new variants. However, it would require a statistically enormous number of people to get the virus before they could produce a new variant by chance. This is because a mutant virus particle will only make up a small portion of the virus population inside a person's body. Therefore, it is highly unlikely that this particular particle will be able to spread to a new person. Whereas, in the vaccinated, their weak immune response specifically selects for the mutant variants. It is highly likely that if a vaccinated person passes on the virus to another person, the particles they pass on will be those that have the ability to escape from the immune response elicited by the vaccines. An analogy would be if you did an experiment with 500 room temperature petri dishes filled with bacteria and 500 heated petri dishes with bacteria, then found a heat resistant variant but didn't know which dish it came from. It would be absurd to think that the heat resistant strain of bacteria came from the room temperature petri dishes. It would possible, sure, but completely improbable that the heat resistant strain had suddenly appeared in a room temp petri dish. There would be no reason for it to become a dominant strain in that environment. Logically, statistically, and evolutionarily, it must have come from the heated petri dishes. This is a very basic and obvious conclusion, but the media and government bureaucrats in lab coats are trying to tell you that the absurd thing is true. They're trying to say that the unvaccinated (the room temperature petri dishes) are where the vaccine resistant strains are coming from.
Geert Vanden Bossche is a virologist who has been sounding the alarm on this issue, you can visit his website or see a full collection of his videos down below: https://www.geertvandenbossche.org/
Evidence of cov2 immune escape: https://science.sciencemag.org/content/early/2021/06/30/science.abi7994
Article from 2015 that explains how imperfect vaccination (like the Pfizer and moderna that require at least two shots to be effective) can create immune escape variants: https://journals.plos.org/plosbiology/article?id=10.1371/journal.pbio.1002198
Article from 2021 explains that unless vaccination is done quickly, there will be a high probability of escape mutants: https://www.nature.com/articles/s41598-021-95025-3
CDC warns COVID-19 may be a few mutations away from evading vaccines. The virus isn't mutating to avoid the vaccines because of unvaccinated people, it's because the vaccines are putting evolutionary pressure on the virus: https://nypost.com/2021/07/27/cdc-covid-19-may-be-a-few-mutations-away-from-evading-vaccines/
3. Antibody Dependent Enhancement
There is a potential for ADE, antibody dependent enhancement. This is when the virus mutates so that the antibodies no longer neutralize the virus but the antibodies still try to attach to it. This can actually help the virus get into your immune cells because when the virus is covered with antibodies it will draw macrophages to the virus that will try to eat it. However, when your macrophages come to eat the virus particle that they think has been neutralized, the virus gets inside them and starts replicating because the antibodies actually didn't neutralize the virus. Your own antibodies act like a kind of Trojan Horse. Another way that ADE can happen is your own antibodies connect to the receptors of your cells and actually help the virus get in directly. This was a huge problem with the Dengue vaccine and we need to do a lot of testing to make sure this isn't a possibility. Clearly with these rushed vaccines we haven't eliminated this possibility and with the virus mutating, ADE may pop up with a later variant. We must stay vigilant and keep an eye out for this signal. It will manifest as people with high antibody levels being more likely to get sick and die.
Journal article from 2005 shows evidence that sars-cov1 vaccine, that also focused on the spike protein, caused ADE when subjects were challenged with different strain: https://www.nature.com/articles/news050110-3#ref-CR1
Article explaining how ADE works in Sar-cov1: https://www.nature.com/articles/s41586-020-2538-8
Article explaining the potential for ADE in Covid19: https://www.nature.com/articles/s41586-020-2538-8
Another article that speculates on the potential for ADE in Covid19: https://pubmed.ncbi.nlm.nih.gov/32920233/
Article explaining the potential risks of ADE in Sar-cov2: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7943455/
Article from 2021 explains that there is evidence that covid19 is able to kill macrophages by using antibody dependent mechanisms: https://www.biorxiv.org/content/10.1101/2021.02.22.432407v1
Paper explains that the delta variant is extremely close to developing the ADE, only a few mutations will allow it to use our own antibodies to enter our cells: https://www.biorxiv.org/content/10.1101/2021.08.22.457114v1
4. The Potential for Autoimmune Disorders
There is a potential for an autoimmune response from the vaccines. The vaccines that were developed for Sars-Cov-1 used the spike protein, just like the vaccines for Sars-Cov-2. Unfortunately, the old vaccines caused the animals to develop serious autoimmune disorders and causing severe organ damage. There is a question about whether these new vaccines, which also focus on the spike protein, will also cause autoimmune disorders. Since both the old vaccines and the new vaccines utilize the spike protein to elicit an immune response, there is a danger that the new vaccines will have the same issues. The problem is that autoimmune disorders take a long time to develop and to be detectable. It may take a long time before doctors and scientists can link the sudden rise in certain kinds of autoimmune disorders with these vaccines. Usually, in a vaccine trial you closely monitor your trial group for years and years. This allows you to identify the signals. With the current program of injecting millions of people, there will be no clear way to link causation to the vaccines and an increase in autoimmune disorders may just fly under the radar. We may not know for a very long time or we may never know. Another concern is that because of the way the mRNA vaccines work, they cause your own cells to present as foreign entities. Your immune system comes over and starts killing your own cells. This has never been done before in human history. We have no idea if there will be long term consequences for teaching your immune system to treat its own cells as foreign material. We will have to wait and see whether this will lead to autoimmune disorders. This means that caution, at the very least, is justified and rational.
Journal article from 2004 on autoimmune disorders from Sars-cov1 vaccine that also focused on the spike protein: https://www.cidrap.umn.edu/news-perspective/2004/12/sars-vaccine-linked-liver-damage-ferret-study
Journal article from 2005 on autoimmune disorders from Sars-cov1 vaccine that also focused on the spike protein: https://pubmed.ncbi.nlm.nih.gov/15755610/
Journal article from 2012 on autoimmune disorders from Sars-cov1 vaccine that also focused on the spike protein: https://journals.plos.org/plosone/article?id=10.1371/journal.pone.0035421
Journal article from 2020 on autoimmune disorders from Sars-cov vaccine (can't figure out if they're talking about cov1 or 2): https://jvi.asm.org/content/78/22/12672.abstract
Journal article from 2020 explains why immune disorders happen with covid vax, because human and Covid19 proteins are similar: https://www.sciencedirect.com/science/article/pii/S2589909020300186
5. The Narrow Design Focus of the Vaccines and Lack of Efficacy
The mRNA vaccines are narrowly focused on just the spike protein when they could have been designed to target more proteins. The Covid19 coronavirus has 4 main proteins. There are 3 on its outside and 1 on the inside. The S-protein, the M-protein, and the E-protein, are on the outside, while the N-protein is on the inside. When you get a natural infection your body will likely produce antibodies for all or most of these proteins (depending on the function of your own unique immune system). We knew from studying Sars-Cov-1 that antibodies to the S-protein and the M-protein are both neutralizing. In fact, they used exactly that knowledge when they designed the current vaccines. So, they could have tried to make vaccines that utilize the M-protein to avoid the potential for autoimmune disorders discussed above. But they didn't, they instead focused only on the S-protein. They could have designed the vaccines so that they present both the S-protein and the M-protein. This would have made the vaccines much more effective and less leaky since any mutated virus particles would have to have mutated both the S-protein and the M-protein to avoid the antibodies. Whereas, the current vaccines are narrowly focused on just the S-protein, meaning that the virus only has to mutate the one protein. It is exponentially harder for an organism to mutate two beneficial traits vs just mutating one beneficial trait. So, these vaccines are worse than they could have been. We are seeing the results of these mediocre medications in the data coming from highly vaccinated countries.
Article explains how vaccine manufacturers have used relative risk reduction to determine that vaccine efficacy is ~90+%, however they should have used absolute risk reduction which would tell us that the vaccines will only reduce total covid cases by ~1%: https://www.thelancet.com/journals/lanmic/article/PIIS2666-5247(21)00069-0/fulltext
Addendum to the above information. This video from 2013 explains the difference between relative and absolute risk reduction in a very simple way: https://www.youtube.com/watch?v=7K30MGvOs5s&ab_channel=TerryShaneyfelt
Article from 2005 explains that antibodies to the S-protein and the M-protein are effective in neutralizing the sars-cov1 virus. However, the sars-cov2 vaccines only target the S-protein. This is evidence that the vaccine manufacturers could have chosen to make a superior mrna vax that produced two types of antibodies, but chose to focus narrowly on just the S-protein: https://pubmed.ncbi.nlm.nih.gov/16544518/
Antibodies from vaccines start to drop within 6 months, get ready for endless boosters: https://www.nature.com/articles/s41586-021-03777-9
Iceland covid data shows majority of covid cases are fully vaccinated: https://www.covid.is/data
UK data for August 2021 shows 183,000 unvaccinated cases with 390 deaths, and 73,000 vaccinated cases but with 679 deaths. So, it seems that getting vaccinated reduces your chances of getting covid, but increases your chances of dying from it if you do get it: https://assets.publishing.service.gov.uk/government/uploads/system/uploads/attachment_data/file/1012644/Technical_Briefing_21.pdf
Vaccinated healthcare works who experienced a vaccine failure still had huge viral loads: https://papers.ssrn.com/sol3/papers.cfm?abstract_id=3897733
Pfizer intentionally destroyed the control groups in their trials for the covid vaccine, which means we'll never know how effective the vaccine actually is: https://www.npr.org/sections/health-shots/2021/02/19/969143015/long-term-studies-of-covid-19-vaccines-hurt-by-placebo-recipients-getting-immuni
Moderna has never been able to get a drug or vaccine approved by the FDA, they were chosen by Trump because the CEO said they could get their experimental gene therapy vaccine made in the fastest time, no animal trials were done: https://www.cnn.com/2020/05/01/us/coronavirus-moderna-vaccine-invs/index.html
Moderna CEO Stephane Bancel explains that they designed the vaccine in just two days: https://v.redd.it/p83r1m7zzgd71
Even CNN agrees the rushed vaccine is a stupid idea (but only while Trump was president): https://edition.cnn.com/2020/09/01/health/eua-coronavirus-vaccine-history/index.html
6. There are Alternatives to Vaccination
There are alternative treatments that are effective against Covid19 but they are being suppressed. Why? Because the vaccines are not approved by the FDA but instead they are emergency use authorized only. The emergency use authorization can only be granted if "there are no adequate, approved, and available alternatives". Well, a growing body of scientific research is showing that both Ivermectin and Fluvoxamine (among other drugs) are adequate alternatives for early treatment of Covid19, and both of these drugs have been FDA approved for years. Unfortunately, that means they are now off patent and no one can make any money off of them. So, for the vaccines to continue to receive their EUA, the existence of these treatments must be suppressed. We have seen a huge amount of censorship of doctors who have been speaking out about these drugs.
Ivermectin
Emergency use authorization for the vaccines cannot be granted if there are effective alternative approved treatments for Covid19. So, if the pharmaceutical industry is going to make any money off covid, they must suppress the existence of any existing off patent drugs that may be effective in treating or preventing covid: https://www.fda.gov/emergency-preparedness-and-response/mcm-legal-regulatory-and-policy-framework/emergency-use-authorization
Meta-analysis on the efficacy of Ivermectin in treating Covid19: https://journals.lww.com/americantherapeutics/Abstract/9000/Ivermectin_for_Prevention_and_Treatment_of.98040.aspx
A double-blind, randomized placebo-controlled trial shows that Ivermectin is able to significantly reduce viral load within 6 days for most people: https://www.medrxiv.org/content/10.1101/2021.05.31.21258081v1
More evidence that Ivermectin treatment leads to much faster recovery from Covid19: https://onlinelibrary.wiley.com/doi/10.1002/jmv.26880
A study reveals that a five-day course of ivermectin for the treatment of COVID-19 may reduce the duration of illness: https://pubmed.ncbi.nlm.nih.gov/33278625/
Ivermectin stops replication of covid: https://www.sciencedirect.com/science/article/pii/S0166354220302011
Ivermectin has anti-viral properties: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3888155/
Ivermectin has anti-viral properties against covid: https://www.nature.com/articles/s41429-020-0336-
Ivermectin binds to Covid19 proteins to block the virus: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7996102/
Evidence that Ivermectin can be effective as a prophylaxis, Argentinian frontline healthcare workers were given Ivermectin as a preventative and zero got sick with covid, whereas 58.2% of the control group who did not take Ivermectin got covid: https://www.buongiornosuedtirol.it/wp-content/uploads/2021/04/Nota-Journal-of-Biomedical-Research-Safety-and-Efficacy-Iota-Carrageenan-and-Ivermectin.pdf
Ivermectin safe to give 12mg per day for 5 days: https://www.ijidonline.com/article/S1201-9712%2820%2932506-6/fulltext
Ivermectin safely administered 60mg per day for 6 months: https://www.tandfonline.com/doi/full/10.1080/10428194.2020.1786559
Fluvoxamine
Fluvoxamine helps in covid treatment: https://pubmed.ncbi.nlm.nih.gov/33180097/
Covid leads to long term inflammation, useful for long haul Covid19 treatment: https://pubmed.ncbi.nlm.nih.gov/33391730/
Fluvoxamine has anti-inflammatory properties that can help treat covid: https://www.frontiersin.org/articles/10.3389/fphar.2021.652688/full
Fluvoxamine targets sigma-1 to stop covid replication: https://pubmed.ncbi.nlm.nih.gov/33403480/
7. They are Pushing the Vaccine on People Who Clearly Don't Need It
We've known for decades that once you are infected with a virus or disease, your body creates a robust immune response, including memory T cells and B cells. These cells stick around so that you can quickly respond to a new infection. However, this fact is being completely ignored by vaccine pushers. They want a needle in every arm, even in the arms of those who do not need it, like the covid recovered. We might say, well covid is new and different, and perhaps immunity wanes after a time. This assumption was prudent in the beginning of the pandemic but now we have lots of evidence that the covid recovered have a near zero chance of getting sick again. Your body takes a few weeks and months to build up its antibodies after an infection. During this time your body is susceptible to a second infection. Most of the time when a second infection takes place, it occurs during this time of antibody build-up. There is no reason to force every covid recovered patient to take an invasive experimental drug, especially after that initial 3 month period after they have built up a sufficient immune response. If you still think that the miniscule chance that their immune system has failed makes them a danger, then why are these people not asked for proof of antibodies? It's because they don't actually care if you have antibodies. The vaccinated, without knowing whether they have antibodies or not, can walk around freely touching vegetables and sharing drinks, but a covid recovered patient, with proof of antibodies is still considered a biohazard. This is backass wards and it is evidence that vax pushers don't actually care about immunity. It is just about getting a needle into every arm. The reason why they are doing this, I do not know. I leave it up to you to speculate. But it doesn't make sense and I make a point of not going along with things that don't make sense.
No benefit from vaccination for previously infected individuals: https://www.medrxiv.org/content/10.1101/2021.06.01.21258176v2
Covid19 infection produces long lasting immunity: https://www.nature.com/articles/s41586-021-03647-4
Second article that covid19 infection produces life long immunity: https://www.nature.com/articles/d41586-021-01442-9
More evidence that covid19 infection produces long term immunity: https://www.medrxiv.org/content/10.1101/2021.04.19.21255739v1
Study of 600,000 covid recovered patients finds less than 1% reinfection rate over 10 months and an almost 0% risk in the first 7 months: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8209951/pdf/RMV-9999-e2260.pdf
8. The Growing Evidence of Adverse Reactions to the Vaccines and the Censorship of this Evidence
There is a growing amount of data that people are having severe reactions to the vaccines. It gets little to no coverage in the press, in some cases people who talk about their reactions on social media are being censored and called anti-vaxxers (I mean, how asinine to call someone who took the jab an anti-vaxxer) or fakers (I am sure some are faking for money/attention, but I highly doubt it's many of them given the social consequences for lying). Some senators have done press conferences with these vaccine harmed people so they can tell their stories. Some doctors have spoke out, although many are being censored and threatened with losing their licenses. Some internet platforms are still allowing people to tell their stories. But many communities are being deleted or shutdown. I remember when journalists, data scientists, and doctors were sounding the alarm on covid in January 2020 while all the authorites and big shot scientists were saying "no, no, everything is fine, it's just the flu bro, go hug a Chinese person, or are you a racist". What if those people had been censored then? Many of the same people who alerted us to covid are sounding the alarm on these vaccines now. We were lucky then that they were not censored. We are lucky now that there are publicly accessible government databases which contain reports of people who have had adverse reactions to the vaccines. These systems were put in place in the 90's to act as an early warning system and to give transparency to the public after previous botched vaccine rollouts, like the 1976 swine flu vaccine debacle. You can go and read these reports of adverse reactions to the vaccines for yourself. There are websites that download the reports and present them to the public in a very readable manner (the government website from the 90's is not very good). There are concerns that these reports are being made in error or by bad actors. However, research has been done into these systems and it was found that 86% of the adverse reactions had seemingly no other cause or explanation aside from the covid vaccine. In the past, if a vaccine hit 50 deaths or a few hundred adverse reactions on these reporting systems, they would shutdown the vaccination program. As of writing this, for the covid vaccines, the deaths in the US are above ten thousand and the serious adverse reactions are into the hundreds of thousands. Yet they just keep rolling with the shots and are even forcibly mandating them.
Analysis on the VAERS death data shows that in 86% of reports the vaccine cannot be ruled out as a causal factor in the death of the patient: https://www.researchgate.net/publication/352837543_Analysis_of_COVID-19_vaccine_death_reports_from_the_Vaccine_Adverse_Events_Reporting_System_VAERS_Database_Interim_Results_and_Analysis
Addendum to the above link. OpenVAERS is a site that allows you to easily read VAERS reports and breaks down the numbers. The reports seem to be a lot of people who have comorbidities or are old, but there are also some really eye opening cases where young people experience horrible side effects. Read for yourself and make up your own mind about what the vax is doing to your fellow Americans: https://www.openvaers.com/openvaers
9 & 10 Continued in the Comments
2020.12.24 22:17 mortois1 How the Covid mRNA vaccines work - a Santa Claus analogy
There has been a lot of misinformation going around about the Covid vaccines currently being deployed, and a lot more good-intentioned skepticism. Will the vaccine give you covid? Will it make me sick? Will it alter my DNA? Most of this skepticism and fear is due to not simply not understanding how these vaccines actually work. I thought I’d take a few paragraphs to try to put it into seasonally appropriate terms, using everyone’s favorite metaphor - Santa Claus.
Imagine your cells are Santa’s workshop.
Santa is your DNA, and he works in his office in the middle of the workshop. The nucleus.
Outside of his office, the workshop is full of tiny little elves, also known as your ribosomes.
Santa has a big book of toy schematics, and as Christmas approaches he makes copies of designs from this book, or mRNA, and sends them out of his office to his elves.
His elves use these designs to make toys. The toys then get sent out of the workshop to be distributed among the children of the world.
The children are your immune system.
Children, of course, know a good toy when they see one. They watch commercials, they see ads, they have the YouTube. So when they see a Barbie, or a GI joe, or a baby yoda doll, or a PS5 they recognize it and greedily welcome it into their home.
But one day someone sneaks a design for brussel sprouts into Santa’s workshop. The mRNA vaccine.
It stays out of his office, so it never makes it into Santa’s book, and the old man is none the wiser.
But outside on the factory floor, the elves get a hold of it, and since it looks like any other toy design, they start churning brussel sprouts out by the thousands. They then place them onto Santa’s sleigh, where he deposits them into stockings all over the world.
But when the kids of the world upend their stockings and a few brussel sprouts roll out, they sense something is wrong.
They reject the brussel sprouts. They attack the brussel sprouts. They stomp on them, they crush them in their creepy little fists, they throw them at the cats. (The cats are representative of nothing in my analogy, they just had it coming)
Most importantly, since the kids like to use the TikTok, they record video snippets of this travesty which disseminate around the world. It takes a while for the word to spread, but eventually it does, and next time the kids of the world see a brussel sprout, they will be ready.
TikTok is your T-Cells.
Now, since the children of the world have been made wise, the next time mom and dad try to serve up brussel sprouts, their kids will recognize the devil’s cabbage, cleverly hidden between the meatloaf and the potatoes, and promptly throw the whole plate across the room at the cat.
That’s basically - no, that’s EXACTLY how these mRNA vaccines work. They introduce small pieces of RNA into the cell, and the cell uses that to churn out copies of the “spike protein” which stud the envelope of the coronavirus. The vaccine RNA is then broken down by the cell and goes away. It never enters the nucleus, and never even sees your DNA let alone alters it, and though it makes a piece of a protein on the coronavirus, it neither uses a virus to enter your cells, nor makes any intact virus which could make you sick. But since it does make that protein, and alerts your immune system to its presence, the next time your body sees it on the outer envelope of a coronavirus, it throws the whole virus at the cat.
We are not going to see the end of this pandemic until roughly 70% of us are immune to covid. If that immunity is obtained through infection, it will likely be short-lived, and gained at the expense of millions of lives. Not an option. The only option is vaccination. For vaccination to work, at least about 70% of us need to take the vaccine. That means, technically, 30% of us can skip it and ride along on the coattails of those who were vaccinated. But if 50% of us decide to be the 30%, we all lose. That’s why, even though you might not want to take the vaccine, you should take the vaccine. You may not like it, but sometimes you just have to eat your brussel sprouts.
submitted by mortois1 to CovidVaccine [link] [comments]
Imagine your cells are Santa’s workshop.
Santa is your DNA, and he works in his office in the middle of the workshop. The nucleus.
Outside of his office, the workshop is full of tiny little elves, also known as your ribosomes.
Santa has a big book of toy schematics, and as Christmas approaches he makes copies of designs from this book, or mRNA, and sends them out of his office to his elves.
His elves use these designs to make toys. The toys then get sent out of the workshop to be distributed among the children of the world.
The children are your immune system.
Children, of course, know a good toy when they see one. They watch commercials, they see ads, they have the YouTube. So when they see a Barbie, or a GI joe, or a baby yoda doll, or a PS5 they recognize it and greedily welcome it into their home.
But one day someone sneaks a design for brussel sprouts into Santa’s workshop. The mRNA vaccine.
It stays out of his office, so it never makes it into Santa’s book, and the old man is none the wiser.
But outside on the factory floor, the elves get a hold of it, and since it looks like any other toy design, they start churning brussel sprouts out by the thousands. They then place them onto Santa’s sleigh, where he deposits them into stockings all over the world.
But when the kids of the world upend their stockings and a few brussel sprouts roll out, they sense something is wrong.
They reject the brussel sprouts. They attack the brussel sprouts. They stomp on them, they crush them in their creepy little fists, they throw them at the cats. (The cats are representative of nothing in my analogy, they just had it coming)
Most importantly, since the kids like to use the TikTok, they record video snippets of this travesty which disseminate around the world. It takes a while for the word to spread, but eventually it does, and next time the kids of the world see a brussel sprout, they will be ready.
TikTok is your T-Cells.
Now, since the children of the world have been made wise, the next time mom and dad try to serve up brussel sprouts, their kids will recognize the devil’s cabbage, cleverly hidden between the meatloaf and the potatoes, and promptly throw the whole plate across the room at the cat.
That’s basically - no, that’s EXACTLY how these mRNA vaccines work. They introduce small pieces of RNA into the cell, and the cell uses that to churn out copies of the “spike protein” which stud the envelope of the coronavirus. The vaccine RNA is then broken down by the cell and goes away. It never enters the nucleus, and never even sees your DNA let alone alters it, and though it makes a piece of a protein on the coronavirus, it neither uses a virus to enter your cells, nor makes any intact virus which could make you sick. But since it does make that protein, and alerts your immune system to its presence, the next time your body sees it on the outer envelope of a coronavirus, it throws the whole virus at the cat.
We are not going to see the end of this pandemic until roughly 70% of us are immune to covid. If that immunity is obtained through infection, it will likely be short-lived, and gained at the expense of millions of lives. Not an option. The only option is vaccination. For vaccination to work, at least about 70% of us need to take the vaccine. That means, technically, 30% of us can skip it and ride along on the coattails of those who were vaccinated. But if 50% of us decide to be the 30%, we all lose. That’s why, even though you might not want to take the vaccine, you should take the vaccine. You may not like it, but sometimes you just have to eat your brussel sprouts.
2020.08.02 21:05 Earthfall10 [Humans are Hiveminds] Pt 10: Lost in Translation
As this is a language of tastes and strands of DNA analog names cannot be written phonetically and are instead replaced with a human name or Earth analog in [brackets].
Span: The diameter of an average [Gaian] = 0.94mm, Kilospan = 0.94m.
Beat: The amount of time takes an average [Gaian] to move their cilia = 0.064s, kilobeat = 1min 4s
Work Cycle: 10 kilobeats. Equivalent to around 15 hours on their time scale
Day: Day length on [Gaia] = 28h 16min. Equivalent to around 3 months on their time scale.
Year: Year length on [Gaia] = 224.4 days = 264.3 Earth days.
[First] [Previous] [Next]
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Alison was removing her report from the scanner when the intern looked up from reading a new message on his screen. “Oh, there is some news you need to hear. The linguists and interrogators have arrived and are being processed at the front desk at the moment, they should be meeting with you shortly. They are also insisting on some security changes.” He paused to type on his keyboard for a second and the scanner began printing a checklist, Alison glanced at it worriedly while the intern returned to skimming the document on his screen. “Ok, some extra guards will be arriving soon and the NSA is insisting the lab with the aliens will need to follow biosafety level 3 protocols. Some guys from the biohazard wing are coming by to give you guys a proper hermetically sealed tank with a filtered air supply to keep the wasps in. They are also going to move that food sample you took to one of their labs.” He said, glancing back up at Alison.
Oh great. That won’t be a test of trust at all Alison thought as she imagined trying to wrangle the wasps into a new cage. Security was probably going to insist on clamping their wings again for that.
She sighed and picked up the fresh printout. “What’s the eta on the new tank?”
Some scrolling and clicking later “Hmm, 10 to 15 minutes. They say they had a wheeled one in storage that they are about to send over.”
“That’s quick at least, I’ll go tell the others to get ready for them. Bye.” She said briskly as she rushed back to the lab and brought the others up to speed. Carl was a bit annoyed about having his sample taken away.
“Really? They are worried about diseases from these guys? They are aliens. That’s worse than worrying about a pine tree catching a cold, at least a pine tree still uses the same biochemistry. These guys don’t even use DNA.” Carl grumbled as he packed his equipment and the sample back up.
“Look, I know it’s unlikely but you know how paranoid people are about this sort of thing, NASA kept the Apollo 11 guys in quarantine for over three weeks just in case there were deadly diseases on the Moon.” Alison grumped back. “Anyway, I need to go tell our guests that their cage is going to be changing soon. I hope they add that water tank we asked for, that might sweeten the deal.” She said over her shoulder as she walked over to the Faraday cage.
——————————————————————
[Walter] was feeling a bit better by now, the giant had been gone for a bit over a cycle and the lack of constant watching had finally let him relax enough that he was willing to shift his focus inwards and fix his broken mind. [Eve] had restored some function to his signaling pathways but she was no surgeon and they were still in pretty rough shape. They were beginning to heal on their own, but it was far too slow.
He knew he had been procrastinating these last few cycles, he really wasn’t keen on messing with his mind weaving equipment again after that last disaster. It was a silly fear, he had worked with those tools for decadays, they were the foundation of his work as an operator, but that almost made the fear worse in a way. That even a trusted tool could kill you if you made a slight mistake. Regardless, he couldn’t keep making up excuses for pushing it off, not if he wanted to control his body well enough to be able to escape if it came to that. At the moment he was pretty sure he couldn’t fly. He glanced around the cage and the room beyond one last time before disconnecting from his craft and turning his attention inwards.
There was the brief bought of disorientation that always comes when swapping between different senses. The arms and tendrils that wove out from the main control center of the weaving equipment were coated in taste and touch sensors, and sensors in each joint fed him a constant sense of each limb’s location. The hundreds of such limbs sprawled about throughout his body flooded him with a torrent of sensory input that was briefly overwhelming. Bringing a few minor thought centers to bear on the data pouring in the noise gradually became understandable and he cautiously sent a few dozen tendrils to examine several of his major motor signaling pathways.
As he felt around he found many treads were still loose, the protein walkways trailing off to nowhere. He could taste memory snippets and pheromone signals piling up along them or falling off into the surrounding fluid, the walker proteins in the water spasming as they blindly repeated their walking cycle with nothing to grab onto. [Walter] [sighed].
About as bad as I thought. Feels like a bit over half of the fibers are still cut. Well, no more putting it off, better get to work.
[Walter] began the slow process of identifying each snipped end and linking them back up to their proper counterpart, triggering ribosomes to manufacture extra cabling to fill in gaps where they didn’t break cleanly. Several kilobeats drifted by as he was lost in the work.
I should really add in some redundant lines and put some safe guards on this thing, I don’t want another situation like that being possible He thought to himself as he finished up the last touches on his 8th motor group. He started planning some upgrades and rereading the mindweaver’s control center programing manual when a signal packet with [Eve]’s scent came in.
“Hey [Walter], you should wake up, [Alison] is back and has some news for us.”
[Walter] grumbled internally for a moment before stowing his equipment, properly this time, and disconnecting. With a jerk his normal senses returned to him and he fiddled with his craft’s comm.
“OK, booting back up now.” He replied, before linking with his craft again. Almost immediately he could feel the improvement, his motor functions weren’t twitching out like crazy in his real body or in the link anymore. Looking around with his craft’s eyes he watched his front legs draw perfect circles in the air with relief.
“You made some progress I take it?” [Frank] asked looking over at him.
“Yeah, I’m mostly back together now. There are still a few more final touchups before I’m 100 percent again, but that should only take a few more kilobeats of work.” [Walter] said, lowering his legs back down and turning to look at the source of his interruption. The colony was standing over their cage again and was looking at a large flexible sheet of white material clutched in one of its grasping limbs.
“What was the news you were talking about [Eve]?” [Walter] asked, turning his attention a bit lower to the craft standing at the front of the cage. [Eve] turned and waved an antenna at him. “Yeah, sorry about interrupting you [Walter], just figured you should know the colonies have decided to move us to a more sealed cage, their leaders are apparently paranoid about diseases. We told them that we don’t have any pathogens in us and none of them could affect them anyway, but apparently they don’t trust us enough to take our word on that.”
“Fair enough.” [Walter] muttered. “I wouldn’t trust them that much either. Though that does make any hope of escape slimmer.”
[Eve] sent a signal of indifference. “Any escape plan would have to involve our craft if we want to survive more than a tenthday and we’d need more than a slight gap in a hatch to get these things out. We already can’t break out of this chamber, another slightly tougher one won’t make a difference. Our best chance to escape would be while they are moving us.”
“Should we make a break for it though?” [Frank] interjected. “They haven’t contacted our ship yet so no one is coming to pick us up yet. We might be able to cobble together a radio powerful enough to reach them, but that’s a really big if depending on where we are. And also let’s not forget the fact we would have to fight our way out of this massive complex with our stingers sealed. That would be suicide.”
“I wasn’t saying we should try and escape now, just that moving between cages is pretty much the only time when that’s an option. Hopefully it will happen again after the ship has been called, or maybe we will get moved to a different facility and can escape while we are outside. But yeah, escaping now would just be dumb, and it could ruin any chances that they might willingly let us go.”
[Walter] thought about interjecting for a moment but decided they had a point and let the matter drop. This new cage story might be a way to trick them into transferring them into testing machines again, but flying away was a dream at this point. He [sighed] and let that dream die.
“OK, we’ll continue playing along for now. When are they going to take us? Are they going to use those blasted clamps again?” He asked, turning to look at the 6 pedestals lined up by the large glass door at the front of the cage, the impassive array of metal limbs and serrated maws atop each glinting in the lamplight.
“I fucking hope not.” Muttered [Eve].
——————————————————————
Alison glanced away from the check list she was rereading as the radio hissed to life.
Hmm, they took a few seconds this time. That’s a bit longer than usual.
“Transfer. When. How.” The radio asked.
“In around 5 minutes.” She said, glancing at a clock. “Oh, that’s one part in 60 of an hour. I don’t know how you will be transferred, that’s probably up to the people setting up the new tank. They might use the clamps again or transfer you in a sealed box. They don’t want you contaminating the air.”
“No. Want. Clamps.”
Alison grimaced. “Understandable, sorry about that. Though it would be a good chance for me to add some marking on you.”
“…Why” The radio hissed after a moment.
“Ah, because I have trouble telling you apart.” Alison said slightly embarrassedly. “You also all use the same voice so it’s hard to know who’s speaking. I assume it’s you up front?” She asked, pointing at the wasp up at the front with its antenna on the glass.
“Yes.” The radio hissed. “Try. Fix. Sound.”
“What do you mea-“ Alison paused as the radio began talking with its voice clips shifted into a higher pitch.
“Different. Speaker.” It squeaked.
Alison managed to keep a straight face and replied. “That helps a bit, but telling 8 different pitches apart, especially given the range of voices you guys use for each sound clip, would be pretty hard. How about you send on different radio frequencies and I’ll set up a display to show whose talking.”
“Yes.”
Alison spent a few moments plugging a tablet into the radio and setting up an audio app to display eight different channels. “Ok, I have this set up, send me the different frequencies you’re going to use and identify yourselves.”
A few seconds of pings followed by legs being raised and she had each one of the bugs set up with a number. Let’s hope I don’t lose track of which is which. She thought as she turned her attention to number 1 at the front of the cage. “Ok, this is working now. This will defiantly help the linguists too. We should get some more radios and let you have multiple conversations going.” She said, adding a note to her next report.
A knock on the door signaled the arrival of the biohazard team. They wheeled in a slightly larger tank with a large box with vents protruding from one side. One of the heavily garbed workers stepped forwards and addressed the collected scientists.
“You will need to undergo decontamination procedures and don proper PPE before you can continue working. We have set up a chemical shower down the hall and a changing station for your equipment. As you have already been exposed we will be monitoring you for any signs of infection, and you will be quarantined to this lab and several sealed off rooms we have been setting up in this wing. The linguists and interrogators from the NSA will be arriving shortly, as you are possibly infected you will make no contact with them. We will be handling any biohazardous materials.”
“How will you be handling the aliens?” Asked Alison.
“We will be transferring them in this case.” The technician said, gesturing to a small box that could fit in one of the tank’s airlocks. “Will they cooperate?” He asked.
“I will ask them to, but that’s all I can really say on the matter.” Alison said cautiously. She turned back to the cage on the desk. “These people will be transferring you in a box now, no clamps. They are going to be putting you in that bigger box there. Will you get in when they tell you?”
“Yes.”
Alison turned to the technician and shrugged. “They have been mostly honest so far but have admitted that they know what lying is. They aren’t openly hostile to the idea at least.”
“Alright, we will handle things from here. You all need to go begin decontaminating.”
The scientists sighed slightly and filed out to the shower. After changing into back-tying gowns, masks and face shields they were given a quick test of their vitals and begrudgingly allowed to get back to work.
“It could be worse.” David grumbled as he fiddled with his gown. “They could have declared BSL-4 and required we all wear positive pressure suits.”
“I just hope they didn’t traumatize any of them.” Deborah muttered as they pushed open the lab door and checked on the wasps.
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[Frank] watched these new colonies warily as they began setting up the room they just wheeled in. They looked odd and mishappened at first until he realized they were wearing some sort of full body covering. One of them stood up clutching a smaller room with one hand, if by small you meant several stories high, but that was practically normal at this point. He guessed this was the box the colonies had been talking about a few kilobeats ago. The creature slowly lumbered past their cage to the huge door on the wall a few kilospan away. Some creaks and groans could be heard as the being shuffled around in whatever chamber was back there before one of the hatches on the back wall clicked open and the box it had been holding slid out, its door ajar. One of the other creatures stood nearby looking in at them and said “Enter” “Bring” “Tool”, pointing at their communication device. [Frank] looked at it curiously. “We can’t lift that.” He replied.
“No” “Small” “You” “Tool”
“Oh, the interface tool, yeah we’ll bring it.”
[Frank] looked around at what was left of their team and sent. “Ok people, let’s get this over with.” He flew over to the new chamber and walked inside cautiously, seeing and smelling nothing amiss. It was just a smaller plastic room. He relaxed slightly and called the others in after him. A few beats later the rest of the group flew in and waited. The creature watching them made a sound and the hatch to the airlock the box was in slid closed. Another hatch behind them opened a sliver and a whirring was heard as the door on their box slid shut. Once their box was sealed the hatch behind them opened up all the way and they could see the colony from before putting away a device on its belt. Massive limbs reached out and picked up their box, with both hands this time, and the creature slowly carried them out into the main room. It seemed to be trying to keep them steady, there was only a slow rocking where it failed to perfectly compensate for its gait.
A few dozen beats later and they were set down in front of the door to the larger cage, much to [Walter]’s relief. The creatures rather unceremoniously slid them inside and shut the door, before fiddling with several devices, flicking beams of light over them, the new cage and the colony which carried them. At last they seemed to be satisfied and one of them flicked a device and their box’s door opened again.
This cage isn’t comm shielded then. That’s useful to know. [Frank] thought as he carefully crawled out. After a slightly longer check of this new space he found little of note. It was a mostly empty reinforced glass box with some fans behind a secure vent whirring in a high corner. He wondered if their request for a water tank had fallen through. There was one other thing in the box with them though, a larger communications device connected to a black box. “What is that?” He asked one of the creatures watching them. They didn’t respond and he realized the radio hadn’t sounded, they were several kilospans away from it now. He grumbled for a bit as the creatures began washing things down instead of setting the radio back up. After a few hundred beats of waving at them fruitlessly he gave up and went back to the smaller box with the others. He was pretty sure the strange black cube wasn’t anything dangerous but there was no reason to test that.
After heading back in he found the fabricator pair had passed the time making some paints from plastic chips they had squired away. “What’s that for?” He sent curiously as he watched them pour out some of the thick grey liquid into a bowl. “It’s body paint so that the humans can tell us apart better.” One of them said. “We can write the numbers our comms are using on our backs.”
“Hmm, I’m not sure if their sight is good enough to distinguish symbols that small from a kilospan away.” [Frank] mused. “You saw how big the symbols on their screens are and they hold those half a kilospan away from their heads’ at most.”
The pair deflated slightly before one perked up “We could do colors instead, that should be clearer than trying to tell apart different squiggles.”
[Frank] sent a signal of cautious acceptance. “If you can make some safe dyes with the chemicals you have on hand you can try. [Alison] seemed to find telling us apart important, it might help them relate to us more.”
“Or they just want to keep track of us better.” [Erin] sent.
[Frank] [shrugged] “Or that. I still think it’s worth it.”
He glanced around at the others who sent signals of acceptance or indifference. A kilobeat latter the fabricators had settled on several dyes that worked in the human color range and made a few different mixes. Each team member soon had a bold stripe running down their crafts abdomen and a splotch on their thorax and head. [Frank] glanced up at the colonies again and saw they were still cleaning. He [sighed] and prepared himself for another long wait.
After a cycle or so of boredom their familiar creatures finally lumbered back in. They were a bit hard to recognize at first due to changing their outer covering and partly obscuring their heads with protective gear but that group of heights, eyes and head filaments was somewhat recognizable.
Oh thank the depths. Maybe now we will get the radio working again.
——————————————————————
Alison scanned the room and saw the new tank up against one of the tables in the middle of the lab.
“How was the transfer?” she asked as she and Deborah walked over. The creatures remined silent which was odd, but one of them flew up and began gesturing at the far end of the room.
Wait, why is it covered in paint? Alison thought before turning to look at where it was pointing.
Oh, they left the radio over there, that was dumb.
Alison walked over to the old cage and grabbed the radio set. “Hey, when did you paint the wasps? I thought you were only going to move them while we were gone?” She asked annoyed to one of the hazmat suited technicians working nearby. He didn’t look up from the door knob he was scrubbing. “We didn’t do that. It just showed up on them after a few minutes, figured they made it themselves somehow. We would like a sample of it soon for safety testing.”
“Oh. That’s interesting. I’ll go ask them about it.”
She finished moving the radio equipment and tablet to the new desk and turned it on.
“Word. Yes.” It said immediately. She glanced at the tablet and say it was number 1 speaking as usual. She smiled slightly, “You missed being able to talk huh?”
“Yes. Boredom. Speak. Work. Help. Return. Vessel.”
“Yes, if you help we might get you to your ship. We have made some progress on that, we have found one of your ships. We will contact them soon, our decision makers really want to talk to them.” Alison said as she got the tablet’s stand propped up.
“Good. When.”
“As soon as some translators arrive and give you more words so you tell them a bit more about what those ships’ reaction might be.”
“Understood.”
Alison glanced around at the wasps cluster around the little transport box, noting the odd shades of color they had dabbed on themselves. “Did you add the colors?”
“Yes. Help. Distinguish.”
Alison grinned “That’s great. Where did you get them?”
“Made.” A purple striped drone said, holding up a chip of phone casing.
Note to self, they have advanced chemical plants in those things. Alison thought uneasily.
She spent a few moments relabeling their radio channel names with their colors as the linguists arrived.
——————————————————————
Clark had been waiting in the lobby for 20 minutes now and was struggling to contain his impatience. Real aliens, I’m about to talk to real fucking aliens. He thought with a mix of giddy excitement and disbelief. He glanced annoyedly at the other two agents who had been driven here with him, Hank and Michel he was pretty sure. They were looking of into the distance with rather stonier expressions. They are probably just looking at this as a security threat. Which, I mean, it is. They were spying on us for days, that’s not a great sign. But come on people, we just answered the greatest question in astronomy, have a bit of wonder in your lives. He composed himself as the guard standing at the lobby door checked his ear piece and headed over to them. Clark stood up out of the surprisingly uncomfortable chair he had been sitting in with relief as the guard gestured for them to follow.
Several locked doors and an elevator ride down into the Earth later and they arrived at the wing of the lab where the aliens were being held. The hallway leading up to it was filled white plastic sheets, pumps, plastic tubing, and the harsh smell of cleaning chemicals. “This facility was chosen due to this section being equipped to study electronic warfare equipment.” Their terse guide informed them as they reached the end of the hall and he pointed at the pair of wire laced doors set there. “Each lab room in this wing are Faraday shielded and have their own air gapped servers to prevent any damage to the rest of the facility. You will be provided with digital and analog recording equipment inside the lab, and you will be permitted access to its server, but you are not allowed to bring any digital equipment or recordings out. The only communication with the rest of the lab is carried through these doors as heavily proofread physical printouts or word of mouth. Am I understood?”
Clark and the two other NSA agents nodded; he had been preparing for something like this. “Any external communications will be conveyed to you via a messenger” The guard continued, pointing at a thin man sitting at a desk nearby. The messenger gave them a half-hearted wave and the guard turned back to the group. “In addition to the data security of this room we are modifying it to be compliant with biosafety level 3 protocols due to the discovery that the subjects are alien lifeforms. Disease compatibility is unknown at this time. A changing booth has been set up down that hall for you to put on the required protective equipment.”
Several minutes of instruction and suiting up followed as the four of them put on their garb and recording equipment. Their guide then lead them back to the signal lock into the lab, and Clark could see more hasty modifications present in it as the small room had been partly filled with a chemical shower. The inner door was covered by a clear plastic sheet that was tapped securely to the doorframe, looking through it he could see basically what he had been expecting, a large white room with work stations and banks of equipment lining the walls and several steel tables arrayed in the center.
The guard walked up and rapped on the glass door through the sheet and a man in hazmat gear opened it, giving them a clearer view. The guard pointed to a group of less heavily suited up scientists. “This is the team that has been dealing with these creatures so far. As they have already potentially been exposed, so you will not enter the room and will observe through this sheeting. Do not open the outer door to this room unless someone in the lab has shut the inner door to maintain data security. You may introduce yourselves.” Their guide finished and stepped back to let the interrogators peer in.
Clark tried to pay attention as the 6 scientists exchanged pleasantries but his attention was grabbed by the cage one of the hazmat suited technicians were rolling over to them, a cage with several wasps in it.
“Those are the creatures alright.” Said a short brown-haired scientist who noticed his shift in focus, he was pretty sure she said her name was Alison. “You’re the linguist then?” She asked.
“Um, yeah.” He said, pulling his eyes away. Michel and Hank must have just finished introducing themselves. He thought, glancing at the two other agents. He cleared his throat. “Yes, I specialize in translating languages and code phrases. I understand these creatures have a limited grasp of spoken English correct?”
“Correct.” A radio hissed.
He whipped his head down and saw one of the bugs in the cage was looking up at him. It had a garish shade of green paint spread on its head and back. “Er, hello.” Clark said, crouching down so they were closer to eye level. “How many words do you currently know?”
“Not. Know. Number. Sound. Know. Number. Picture.” The radio said in a strange broken cadence. The creature then turned to look at Alison and gestured at the tablet and battery bank in its enclosure. “What. Box.” It asked.
“The box next to the tablet? That’s a battery pack.” Alison replied
“Word. Battery.”
“A type of power storage.”
——————————————————————
[Eve] stepped back a bit when she heard that and checked her radiation sensor. Nothing unusual. Ok, it’s not one of their more insane types of power source at least.
“What type of power” She asked. She waited for a few hundred beats as the creature above slowly drawled out “Chemical” “Similar” “Communication” “Machine”
She glanced towards [Frank] who [shrugged]. “Sounds like they’re saying it’s a bigger version of their comm unit power sources. Those are somewhat primitive chemical batteries; they are flammable but otherwise pretty safe.”
“All right, if your sure its not going to bust into flames I guess we can turn that bigger device on then. Hopefully it works similarly.”
——————————————————————
Clark watched as the wasps flew over to the tablet and flicked it on. It was already set up and had a drawing app on the home screen.
“Someone suggested a bigger screen and some better apps would be useful.” Said one of the technicians when Alison gave him a questioning look.
After a few moments of clicking around the wasps seemed to get a hang of the larger interface and began writing out a number. “1506 words. Not terrible, not fluent either. OK, I am going to do some relevant vocabulary tests, Mr. Michel Anderson here is going to ask you some of the questions that we are thinking of sending to your ship, answer any of them that you can and tell me which words in them you don’t know.” Clark said as the other agent began pulling out files from his briefcase.
Several minutes of questioning followed, until the green painted alien up front waved several legs at them and said “Slow. Much. More. Talk.”
“You want to us to go much slower?” Clark clarified.
“No. Too. Slow. More. Others. Talk.”
“I think they want to speed things up with multiple conversations.” Alison said.
“Yes. You. Much. Slow. Think.”
“Are they saying we’re stupid or that we’re literally slower?” Michel asked annoyed.
“Slower. Think.”
A pair of wasps grabbed their little stylus again and wrote a 90. “Amount. Slow. Think.” The radio hissed.
Clark’s eyes went wide and he looked at Alison who seemed only a bit surprised. “I figured they were a bit faster than us due to how quickly they responded all the time, but 90-fold is pretty crazy. No wonder they always seemed ADHD. We must be driving you mad with boredom.” She said.
“Yes.” The radio replied.
The NSA agents looked at each other with a rather different concern at the front of their minds. That means they have a massive tactical advantage over us, any fight we have with them they could out maneuver us with ease. And the spying, they have been studying us for a bit over a week at least, that’s multiple years to them. They must know far more about us than we imagined. Clark thought with mounting panic. Our timeline is going to need to be sped way up for this.
He looked at the green bug again “Can your translator understand sped up speech?”
“Yes.”
He turned to the guard by the door. “Get as many people as you can reading this stuff into a microphone and get us a fast audio player.” He said, handing him most of the pile of papers they had prepared. “Also, please for the love of God get us permission to break this signal containment policy. We won’t be able to cram enough people in here to answer their questions in real time, letting people talk to them remotely would speed things up massively. The ships above might come to some decision about us far faster than we thought, we need to start communicating with them today.”
The guard grimaced “I’ll see what I can do.” He said before rushing out the door, papers in hand. Clark tapped his foot impatiently while the technician inside the lab closed the inner door briefly while the guard left, painfully aware that each passing second was a minute and a half to the beings he was trying to communicate with.
What the hell have we gotten ourselves into?
——————————————————————
Director Townsend finished another call with the FBI and sighed as he looked at his freshly filled inbox. At the top was an urgent message from the interrogation team which he clicked open immediately. He reread it twice, paused, and began cursing under his breath. He then made another phone call.
“Yes, this is Townsend again. We have another development. Apparently, these creatures think around 90 times faster than we do. Yes, my response exactly. I am adjusting this lab’s data security policy in light of this, I want an encrypted line of communication to as many trusted linguists as you can get your hands on. This job just got 90 times harder.”
——————————————————————
[Frank] looked on with relief as the creatures seemed to take the revelation of their slowness seriously and were working on a compromise.
“I still think telling them that was a bad idea, that was one of our biggest hidden advantages.” [Erin] grumbled.
“We have been stuck here for two tenthdays already and have only had like 10 conversations. These things have already found one of our ships, we need to get going faster before either of us do something stupid.” [Eve] replied.
[Erin] grumbled to herself for a few beats but didn’t respond and [Eve] let the matter drop. It was a moot point regardless. The things had spent the last few kilobeats rushing around preparing new equipment. From what they could glean from the scattered words they overheard it seemed their leaders were going to let more linguists talk to them remotely. It would still take them kilobeats to answer any questions they asked but there would be multiple colonies working on different questions at once and playing back their answers at high speed. It would be a pain to keep track of which answer was for which question but even still it would speed things up quite a bit.
One of the new colonies, [Clark] was its sound name [Frank] recalled, was setting up a strange folding comm device with dozens of button on its lower surface. He had been plugging in a box with black foam on one side and was pointing it towards them. After some more slow clicks the box began playing quick bursts of sound at them. “You” “Understood” “This”
[Frank] [grinned]. “Yes” he replied. After a few dozen beats the slow creature clicked another button and a sped up recording of one of the creatures asking questions about the voidships began to play.
Now we are getting somewhere.
——————————————————————
Alison watched the linguists setting up equipment on the other side of the plastic screen with a tinge of annoyance that she wasn’t able to help much. She watched the wasps flick about on their tablet, sketching drawings or numbers to answer questions that just sounded like high pitched chirps to her ears. She was recording and monitoring the radio transmissions from and between the creatures on her laptop, slowing it down to see if she could see anything interesting about their language yet. So far it just looked like noise to her, but she figured it would be useful data for the linguists’ latter if they ever wanted to try and speak alien.
Well, send alien radio at least. We would need a DNA printer to ‘speak’ it.
A few hours later and people were beginning to get tired. She checked the clock and saw it was after 8. Shit, already? I hope we are getting paid over time for this…on second thought I hope overtime is still relevant after this. At some point someone from security signed off on giving the creatures the water tank they had requested and the bugs looked like they were taking shifts in it every ten minutes or so, which made sense, the last few hours had been nearly 2 weeks on their scale.
At last at around a quarter to 9 a slightly clearer voice rang out over the radio. “This is Green. We think we have a close good understanding of the language now. We want to talk to vessel now.”
Alison glanced at Clark through the plastic screen and saw he seemed both pleased and a bit apprehensive. Watching your students learn a language in 2 hours will do that to you I guess.
He spent a few moments checking reports from the other linguists they had been messaging with before nodding. “It seems we have covered all of the critical vocabulary we were suggested to, I will inform our leaders of this immediately.”
——————————————————————
Director Townsend downed his fifth cup of coffee for the night as an urgent message from the translation team popped up again. It was good news this time thank goodness. He picked his phone back up and made the big call.
“Townsend again, the translators have just finished and are giving a go ahead on contact. Yes sir. Has the UN made their decision about it yet sir? Yeah that sounds like them alright, but we are still going ahead with it I expect? Of course sir.”
He hung up and sat back in his chair with relief, the project was out of his hands now. For better or for worse humanity was about to make second contact.
[Next]
submitted by Earthfall10 to HFY [link] [comments]
Span: The diameter of an average [Gaian] = 0.94mm, Kilospan = 0.94m.
Beat: The amount of time takes an average [Gaian] to move their cilia = 0.064s, kilobeat = 1min 4s
Work Cycle: 10 kilobeats. Equivalent to around 15 hours on their time scale
Day: Day length on [Gaia] = 28h 16min. Equivalent to around 3 months on their time scale.
Year: Year length on [Gaia] = 224.4 days = 264.3 Earth days.
[First] [Previous] [Next]
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Alison was removing her report from the scanner when the intern looked up from reading a new message on his screen. “Oh, there is some news you need to hear. The linguists and interrogators have arrived and are being processed at the front desk at the moment, they should be meeting with you shortly. They are also insisting on some security changes.” He paused to type on his keyboard for a second and the scanner began printing a checklist, Alison glanced at it worriedly while the intern returned to skimming the document on his screen. “Ok, some extra guards will be arriving soon and the NSA is insisting the lab with the aliens will need to follow biosafety level 3 protocols. Some guys from the biohazard wing are coming by to give you guys a proper hermetically sealed tank with a filtered air supply to keep the wasps in. They are also going to move that food sample you took to one of their labs.” He said, glancing back up at Alison.
Oh great. That won’t be a test of trust at all Alison thought as she imagined trying to wrangle the wasps into a new cage. Security was probably going to insist on clamping their wings again for that.
She sighed and picked up the fresh printout. “What’s the eta on the new tank?”
Some scrolling and clicking later “Hmm, 10 to 15 minutes. They say they had a wheeled one in storage that they are about to send over.”
“That’s quick at least, I’ll go tell the others to get ready for them. Bye.” She said briskly as she rushed back to the lab and brought the others up to speed. Carl was a bit annoyed about having his sample taken away.
“Really? They are worried about diseases from these guys? They are aliens. That’s worse than worrying about a pine tree catching a cold, at least a pine tree still uses the same biochemistry. These guys don’t even use DNA.” Carl grumbled as he packed his equipment and the sample back up.
“Look, I know it’s unlikely but you know how paranoid people are about this sort of thing, NASA kept the Apollo 11 guys in quarantine for over three weeks just in case there were deadly diseases on the Moon.” Alison grumped back. “Anyway, I need to go tell our guests that their cage is going to be changing soon. I hope they add that water tank we asked for, that might sweeten the deal.” She said over her shoulder as she walked over to the Faraday cage.
——————————————————————
[Walter] was feeling a bit better by now, the giant had been gone for a bit over a cycle and the lack of constant watching had finally let him relax enough that he was willing to shift his focus inwards and fix his broken mind. [Eve] had restored some function to his signaling pathways but she was no surgeon and they were still in pretty rough shape. They were beginning to heal on their own, but it was far too slow.
He knew he had been procrastinating these last few cycles, he really wasn’t keen on messing with his mind weaving equipment again after that last disaster. It was a silly fear, he had worked with those tools for decadays, they were the foundation of his work as an operator, but that almost made the fear worse in a way. That even a trusted tool could kill you if you made a slight mistake. Regardless, he couldn’t keep making up excuses for pushing it off, not if he wanted to control his body well enough to be able to escape if it came to that. At the moment he was pretty sure he couldn’t fly. He glanced around the cage and the room beyond one last time before disconnecting from his craft and turning his attention inwards.
There was the brief bought of disorientation that always comes when swapping between different senses. The arms and tendrils that wove out from the main control center of the weaving equipment were coated in taste and touch sensors, and sensors in each joint fed him a constant sense of each limb’s location. The hundreds of such limbs sprawled about throughout his body flooded him with a torrent of sensory input that was briefly overwhelming. Bringing a few minor thought centers to bear on the data pouring in the noise gradually became understandable and he cautiously sent a few dozen tendrils to examine several of his major motor signaling pathways.
As he felt around he found many treads were still loose, the protein walkways trailing off to nowhere. He could taste memory snippets and pheromone signals piling up along them or falling off into the surrounding fluid, the walker proteins in the water spasming as they blindly repeated their walking cycle with nothing to grab onto. [Walter] [sighed].
About as bad as I thought. Feels like a bit over half of the fibers are still cut. Well, no more putting it off, better get to work.
[Walter] began the slow process of identifying each snipped end and linking them back up to their proper counterpart, triggering ribosomes to manufacture extra cabling to fill in gaps where they didn’t break cleanly. Several kilobeats drifted by as he was lost in the work.
I should really add in some redundant lines and put some safe guards on this thing, I don’t want another situation like that being possible He thought to himself as he finished up the last touches on his 8th motor group. He started planning some upgrades and rereading the mindweaver’s control center programing manual when a signal packet with [Eve]’s scent came in.
“Hey [Walter], you should wake up, [Alison] is back and has some news for us.”
[Walter] grumbled internally for a moment before stowing his equipment, properly this time, and disconnecting. With a jerk his normal senses returned to him and he fiddled with his craft’s comm.
“OK, booting back up now.” He replied, before linking with his craft again. Almost immediately he could feel the improvement, his motor functions weren’t twitching out like crazy in his real body or in the link anymore. Looking around with his craft’s eyes he watched his front legs draw perfect circles in the air with relief.
“You made some progress I take it?” [Frank] asked looking over at him.
“Yeah, I’m mostly back together now. There are still a few more final touchups before I’m 100 percent again, but that should only take a few more kilobeats of work.” [Walter] said, lowering his legs back down and turning to look at the source of his interruption. The colony was standing over their cage again and was looking at a large flexible sheet of white material clutched in one of its grasping limbs.
“What was the news you were talking about [Eve]?” [Walter] asked, turning his attention a bit lower to the craft standing at the front of the cage. [Eve] turned and waved an antenna at him. “Yeah, sorry about interrupting you [Walter], just figured you should know the colonies have decided to move us to a more sealed cage, their leaders are apparently paranoid about diseases. We told them that we don’t have any pathogens in us and none of them could affect them anyway, but apparently they don’t trust us enough to take our word on that.”
“Fair enough.” [Walter] muttered. “I wouldn’t trust them that much either. Though that does make any hope of escape slimmer.”
[Eve] sent a signal of indifference. “Any escape plan would have to involve our craft if we want to survive more than a tenthday and we’d need more than a slight gap in a hatch to get these things out. We already can’t break out of this chamber, another slightly tougher one won’t make a difference. Our best chance to escape would be while they are moving us.”
“Should we make a break for it though?” [Frank] interjected. “They haven’t contacted our ship yet so no one is coming to pick us up yet. We might be able to cobble together a radio powerful enough to reach them, but that’s a really big if depending on where we are. And also let’s not forget the fact we would have to fight our way out of this massive complex with our stingers sealed. That would be suicide.”
“I wasn’t saying we should try and escape now, just that moving between cages is pretty much the only time when that’s an option. Hopefully it will happen again after the ship has been called, or maybe we will get moved to a different facility and can escape while we are outside. But yeah, escaping now would just be dumb, and it could ruin any chances that they might willingly let us go.”
[Walter] thought about interjecting for a moment but decided they had a point and let the matter drop. This new cage story might be a way to trick them into transferring them into testing machines again, but flying away was a dream at this point. He [sighed] and let that dream die.
“OK, we’ll continue playing along for now. When are they going to take us? Are they going to use those blasted clamps again?” He asked, turning to look at the 6 pedestals lined up by the large glass door at the front of the cage, the impassive array of metal limbs and serrated maws atop each glinting in the lamplight.
“I fucking hope not.” Muttered [Eve].
——————————————————————
Alison glanced away from the check list she was rereading as the radio hissed to life.
Hmm, they took a few seconds this time. That’s a bit longer than usual.
“Transfer. When. How.” The radio asked.
“In around 5 minutes.” She said, glancing at a clock. “Oh, that’s one part in 60 of an hour. I don’t know how you will be transferred, that’s probably up to the people setting up the new tank. They might use the clamps again or transfer you in a sealed box. They don’t want you contaminating the air.”
“No. Want. Clamps.”
Alison grimaced. “Understandable, sorry about that. Though it would be a good chance for me to add some marking on you.”
“…Why” The radio hissed after a moment.
“Ah, because I have trouble telling you apart.” Alison said slightly embarrassedly. “You also all use the same voice so it’s hard to know who’s speaking. I assume it’s you up front?” She asked, pointing at the wasp up at the front with its antenna on the glass.
“Yes.” The radio hissed. “Try. Fix. Sound.”
“What do you mea-“ Alison paused as the radio began talking with its voice clips shifted into a higher pitch.
“Different. Speaker.” It squeaked.
Alison managed to keep a straight face and replied. “That helps a bit, but telling 8 different pitches apart, especially given the range of voices you guys use for each sound clip, would be pretty hard. How about you send on different radio frequencies and I’ll set up a display to show whose talking.”
“Yes.”
Alison spent a few moments plugging a tablet into the radio and setting up an audio app to display eight different channels. “Ok, I have this set up, send me the different frequencies you’re going to use and identify yourselves.”
A few seconds of pings followed by legs being raised and she had each one of the bugs set up with a number. Let’s hope I don’t lose track of which is which. She thought as she turned her attention to number 1 at the front of the cage. “Ok, this is working now. This will defiantly help the linguists too. We should get some more radios and let you have multiple conversations going.” She said, adding a note to her next report.
A knock on the door signaled the arrival of the biohazard team. They wheeled in a slightly larger tank with a large box with vents protruding from one side. One of the heavily garbed workers stepped forwards and addressed the collected scientists.
“You will need to undergo decontamination procedures and don proper PPE before you can continue working. We have set up a chemical shower down the hall and a changing station for your equipment. As you have already been exposed we will be monitoring you for any signs of infection, and you will be quarantined to this lab and several sealed off rooms we have been setting up in this wing. The linguists and interrogators from the NSA will be arriving shortly, as you are possibly infected you will make no contact with them. We will be handling any biohazardous materials.”
“How will you be handling the aliens?” Asked Alison.
“We will be transferring them in this case.” The technician said, gesturing to a small box that could fit in one of the tank’s airlocks. “Will they cooperate?” He asked.
“I will ask them to, but that’s all I can really say on the matter.” Alison said cautiously. She turned back to the cage on the desk. “These people will be transferring you in a box now, no clamps. They are going to be putting you in that bigger box there. Will you get in when they tell you?”
“Yes.”
Alison turned to the technician and shrugged. “They have been mostly honest so far but have admitted that they know what lying is. They aren’t openly hostile to the idea at least.”
“Alright, we will handle things from here. You all need to go begin decontaminating.”
The scientists sighed slightly and filed out to the shower. After changing into back-tying gowns, masks and face shields they were given a quick test of their vitals and begrudgingly allowed to get back to work.
“It could be worse.” David grumbled as he fiddled with his gown. “They could have declared BSL-4 and required we all wear positive pressure suits.”
“I just hope they didn’t traumatize any of them.” Deborah muttered as they pushed open the lab door and checked on the wasps.
——————————————————————
[Frank] watched these new colonies warily as they began setting up the room they just wheeled in. They looked odd and mishappened at first until he realized they were wearing some sort of full body covering. One of them stood up clutching a smaller room with one hand, if by small you meant several stories high, but that was practically normal at this point. He guessed this was the box the colonies had been talking about a few kilobeats ago. The creature slowly lumbered past their cage to the huge door on the wall a few kilospan away. Some creaks and groans could be heard as the being shuffled around in whatever chamber was back there before one of the hatches on the back wall clicked open and the box it had been holding slid out, its door ajar. One of the other creatures stood nearby looking in at them and said “Enter” “Bring” “Tool”, pointing at their communication device. [Frank] looked at it curiously. “We can’t lift that.” He replied.
“No” “Small” “You” “Tool”
“Oh, the interface tool, yeah we’ll bring it.”
[Frank] looked around at what was left of their team and sent. “Ok people, let’s get this over with.” He flew over to the new chamber and walked inside cautiously, seeing and smelling nothing amiss. It was just a smaller plastic room. He relaxed slightly and called the others in after him. A few beats later the rest of the group flew in and waited. The creature watching them made a sound and the hatch to the airlock the box was in slid closed. Another hatch behind them opened a sliver and a whirring was heard as the door on their box slid shut. Once their box was sealed the hatch behind them opened up all the way and they could see the colony from before putting away a device on its belt. Massive limbs reached out and picked up their box, with both hands this time, and the creature slowly carried them out into the main room. It seemed to be trying to keep them steady, there was only a slow rocking where it failed to perfectly compensate for its gait.
A few dozen beats later and they were set down in front of the door to the larger cage, much to [Walter]’s relief. The creatures rather unceremoniously slid them inside and shut the door, before fiddling with several devices, flicking beams of light over them, the new cage and the colony which carried them. At last they seemed to be satisfied and one of them flicked a device and their box’s door opened again.
This cage isn’t comm shielded then. That’s useful to know. [Frank] thought as he carefully crawled out. After a slightly longer check of this new space he found little of note. It was a mostly empty reinforced glass box with some fans behind a secure vent whirring in a high corner. He wondered if their request for a water tank had fallen through. There was one other thing in the box with them though, a larger communications device connected to a black box. “What is that?” He asked one of the creatures watching them. They didn’t respond and he realized the radio hadn’t sounded, they were several kilospans away from it now. He grumbled for a bit as the creatures began washing things down instead of setting the radio back up. After a few hundred beats of waving at them fruitlessly he gave up and went back to the smaller box with the others. He was pretty sure the strange black cube wasn’t anything dangerous but there was no reason to test that.
After heading back in he found the fabricator pair had passed the time making some paints from plastic chips they had squired away. “What’s that for?” He sent curiously as he watched them pour out some of the thick grey liquid into a bowl. “It’s body paint so that the humans can tell us apart better.” One of them said. “We can write the numbers our comms are using on our backs.”
“Hmm, I’m not sure if their sight is good enough to distinguish symbols that small from a kilospan away.” [Frank] mused. “You saw how big the symbols on their screens are and they hold those half a kilospan away from their heads’ at most.”
The pair deflated slightly before one perked up “We could do colors instead, that should be clearer than trying to tell apart different squiggles.”
[Frank] sent a signal of cautious acceptance. “If you can make some safe dyes with the chemicals you have on hand you can try. [Alison] seemed to find telling us apart important, it might help them relate to us more.”
“Or they just want to keep track of us better.” [Erin] sent.
[Frank] [shrugged] “Or that. I still think it’s worth it.”
He glanced around at the others who sent signals of acceptance or indifference. A kilobeat latter the fabricators had settled on several dyes that worked in the human color range and made a few different mixes. Each team member soon had a bold stripe running down their crafts abdomen and a splotch on their thorax and head. [Frank] glanced up at the colonies again and saw they were still cleaning. He [sighed] and prepared himself for another long wait.
After a cycle or so of boredom their familiar creatures finally lumbered back in. They were a bit hard to recognize at first due to changing their outer covering and partly obscuring their heads with protective gear but that group of heights, eyes and head filaments was somewhat recognizable.
Oh thank the depths. Maybe now we will get the radio working again.
——————————————————————
Alison scanned the room and saw the new tank up against one of the tables in the middle of the lab.
“How was the transfer?” she asked as she and Deborah walked over. The creatures remined silent which was odd, but one of them flew up and began gesturing at the far end of the room.
Wait, why is it covered in paint? Alison thought before turning to look at where it was pointing.
Oh, they left the radio over there, that was dumb.
Alison walked over to the old cage and grabbed the radio set. “Hey, when did you paint the wasps? I thought you were only going to move them while we were gone?” She asked annoyed to one of the hazmat suited technicians working nearby. He didn’t look up from the door knob he was scrubbing. “We didn’t do that. It just showed up on them after a few minutes, figured they made it themselves somehow. We would like a sample of it soon for safety testing.”
“Oh. That’s interesting. I’ll go ask them about it.”
She finished moving the radio equipment and tablet to the new desk and turned it on.
“Word. Yes.” It said immediately. She glanced at the tablet and say it was number 1 speaking as usual. She smiled slightly, “You missed being able to talk huh?”
“Yes. Boredom. Speak. Work. Help. Return. Vessel.”
“Yes, if you help we might get you to your ship. We have made some progress on that, we have found one of your ships. We will contact them soon, our decision makers really want to talk to them.” Alison said as she got the tablet’s stand propped up.
“Good. When.”
“As soon as some translators arrive and give you more words so you tell them a bit more about what those ships’ reaction might be.”
“Understood.”
Alison glanced around at the wasps cluster around the little transport box, noting the odd shades of color they had dabbed on themselves. “Did you add the colors?”
“Yes. Help. Distinguish.”
Alison grinned “That’s great. Where did you get them?”
“Made.” A purple striped drone said, holding up a chip of phone casing.
Note to self, they have advanced chemical plants in those things. Alison thought uneasily.
She spent a few moments relabeling their radio channel names with their colors as the linguists arrived.
——————————————————————
Clark had been waiting in the lobby for 20 minutes now and was struggling to contain his impatience. Real aliens, I’m about to talk to real fucking aliens. He thought with a mix of giddy excitement and disbelief. He glanced annoyedly at the other two agents who had been driven here with him, Hank and Michel he was pretty sure. They were looking of into the distance with rather stonier expressions. They are probably just looking at this as a security threat. Which, I mean, it is. They were spying on us for days, that’s not a great sign. But come on people, we just answered the greatest question in astronomy, have a bit of wonder in your lives. He composed himself as the guard standing at the lobby door checked his ear piece and headed over to them. Clark stood up out of the surprisingly uncomfortable chair he had been sitting in with relief as the guard gestured for them to follow.
Several locked doors and an elevator ride down into the Earth later and they arrived at the wing of the lab where the aliens were being held. The hallway leading up to it was filled white plastic sheets, pumps, plastic tubing, and the harsh smell of cleaning chemicals. “This facility was chosen due to this section being equipped to study electronic warfare equipment.” Their terse guide informed them as they reached the end of the hall and he pointed at the pair of wire laced doors set there. “Each lab room in this wing are Faraday shielded and have their own air gapped servers to prevent any damage to the rest of the facility. You will be provided with digital and analog recording equipment inside the lab, and you will be permitted access to its server, but you are not allowed to bring any digital equipment or recordings out. The only communication with the rest of the lab is carried through these doors as heavily proofread physical printouts or word of mouth. Am I understood?”
Clark and the two other NSA agents nodded; he had been preparing for something like this. “Any external communications will be conveyed to you via a messenger” The guard continued, pointing at a thin man sitting at a desk nearby. The messenger gave them a half-hearted wave and the guard turned back to the group. “In addition to the data security of this room we are modifying it to be compliant with biosafety level 3 protocols due to the discovery that the subjects are alien lifeforms. Disease compatibility is unknown at this time. A changing booth has been set up down that hall for you to put on the required protective equipment.”
Several minutes of instruction and suiting up followed as the four of them put on their garb and recording equipment. Their guide then lead them back to the signal lock into the lab, and Clark could see more hasty modifications present in it as the small room had been partly filled with a chemical shower. The inner door was covered by a clear plastic sheet that was tapped securely to the doorframe, looking through it he could see basically what he had been expecting, a large white room with work stations and banks of equipment lining the walls and several steel tables arrayed in the center.
The guard walked up and rapped on the glass door through the sheet and a man in hazmat gear opened it, giving them a clearer view. The guard pointed to a group of less heavily suited up scientists. “This is the team that has been dealing with these creatures so far. As they have already potentially been exposed, so you will not enter the room and will observe through this sheeting. Do not open the outer door to this room unless someone in the lab has shut the inner door to maintain data security. You may introduce yourselves.” Their guide finished and stepped back to let the interrogators peer in.
Clark tried to pay attention as the 6 scientists exchanged pleasantries but his attention was grabbed by the cage one of the hazmat suited technicians were rolling over to them, a cage with several wasps in it.
“Those are the creatures alright.” Said a short brown-haired scientist who noticed his shift in focus, he was pretty sure she said her name was Alison. “You’re the linguist then?” She asked.
“Um, yeah.” He said, pulling his eyes away. Michel and Hank must have just finished introducing themselves. He thought, glancing at the two other agents. He cleared his throat. “Yes, I specialize in translating languages and code phrases. I understand these creatures have a limited grasp of spoken English correct?”
“Correct.” A radio hissed.
He whipped his head down and saw one of the bugs in the cage was looking up at him. It had a garish shade of green paint spread on its head and back. “Er, hello.” Clark said, crouching down so they were closer to eye level. “How many words do you currently know?”
“Not. Know. Number. Sound. Know. Number. Picture.” The radio said in a strange broken cadence. The creature then turned to look at Alison and gestured at the tablet and battery bank in its enclosure. “What. Box.” It asked.
“The box next to the tablet? That’s a battery pack.” Alison replied
“Word. Battery.”
“A type of power storage.”
——————————————————————
[Eve] stepped back a bit when she heard that and checked her radiation sensor. Nothing unusual. Ok, it’s not one of their more insane types of power source at least.
“What type of power” She asked. She waited for a few hundred beats as the creature above slowly drawled out “Chemical” “Similar” “Communication” “Machine”
She glanced towards [Frank] who [shrugged]. “Sounds like they’re saying it’s a bigger version of their comm unit power sources. Those are somewhat primitive chemical batteries; they are flammable but otherwise pretty safe.”
“All right, if your sure its not going to bust into flames I guess we can turn that bigger device on then. Hopefully it works similarly.”
——————————————————————
Clark watched as the wasps flew over to the tablet and flicked it on. It was already set up and had a drawing app on the home screen.
“Someone suggested a bigger screen and some better apps would be useful.” Said one of the technicians when Alison gave him a questioning look.
After a few moments of clicking around the wasps seemed to get a hang of the larger interface and began writing out a number. “1506 words. Not terrible, not fluent either. OK, I am going to do some relevant vocabulary tests, Mr. Michel Anderson here is going to ask you some of the questions that we are thinking of sending to your ship, answer any of them that you can and tell me which words in them you don’t know.” Clark said as the other agent began pulling out files from his briefcase.
Several minutes of questioning followed, until the green painted alien up front waved several legs at them and said “Slow. Much. More. Talk.”
“You want to us to go much slower?” Clark clarified.
“No. Too. Slow. More. Others. Talk.”
“I think they want to speed things up with multiple conversations.” Alison said.
“Yes. You. Much. Slow. Think.”
“Are they saying we’re stupid or that we’re literally slower?” Michel asked annoyed.
“Slower. Think.”
A pair of wasps grabbed their little stylus again and wrote a 90. “Amount. Slow. Think.” The radio hissed.
Clark’s eyes went wide and he looked at Alison who seemed only a bit surprised. “I figured they were a bit faster than us due to how quickly they responded all the time, but 90-fold is pretty crazy. No wonder they always seemed ADHD. We must be driving you mad with boredom.” She said.
“Yes.” The radio replied.
The NSA agents looked at each other with a rather different concern at the front of their minds. That means they have a massive tactical advantage over us, any fight we have with them they could out maneuver us with ease. And the spying, they have been studying us for a bit over a week at least, that’s multiple years to them. They must know far more about us than we imagined. Clark thought with mounting panic. Our timeline is going to need to be sped way up for this.
He looked at the green bug again “Can your translator understand sped up speech?”
“Yes.”
He turned to the guard by the door. “Get as many people as you can reading this stuff into a microphone and get us a fast audio player.” He said, handing him most of the pile of papers they had prepared. “Also, please for the love of God get us permission to break this signal containment policy. We won’t be able to cram enough people in here to answer their questions in real time, letting people talk to them remotely would speed things up massively. The ships above might come to some decision about us far faster than we thought, we need to start communicating with them today.”
The guard grimaced “I’ll see what I can do.” He said before rushing out the door, papers in hand. Clark tapped his foot impatiently while the technician inside the lab closed the inner door briefly while the guard left, painfully aware that each passing second was a minute and a half to the beings he was trying to communicate with.
What the hell have we gotten ourselves into?
——————————————————————
Director Townsend finished another call with the FBI and sighed as he looked at his freshly filled inbox. At the top was an urgent message from the interrogation team which he clicked open immediately. He reread it twice, paused, and began cursing under his breath. He then made another phone call.
“Yes, this is Townsend again. We have another development. Apparently, these creatures think around 90 times faster than we do. Yes, my response exactly. I am adjusting this lab’s data security policy in light of this, I want an encrypted line of communication to as many trusted linguists as you can get your hands on. This job just got 90 times harder.”
——————————————————————
[Frank] looked on with relief as the creatures seemed to take the revelation of their slowness seriously and were working on a compromise.
“I still think telling them that was a bad idea, that was one of our biggest hidden advantages.” [Erin] grumbled.
“We have been stuck here for two tenthdays already and have only had like 10 conversations. These things have already found one of our ships, we need to get going faster before either of us do something stupid.” [Eve] replied.
[Erin] grumbled to herself for a few beats but didn’t respond and [Eve] let the matter drop. It was a moot point regardless. The things had spent the last few kilobeats rushing around preparing new equipment. From what they could glean from the scattered words they overheard it seemed their leaders were going to let more linguists talk to them remotely. It would still take them kilobeats to answer any questions they asked but there would be multiple colonies working on different questions at once and playing back their answers at high speed. It would be a pain to keep track of which answer was for which question but even still it would speed things up quite a bit.
One of the new colonies, [Clark] was its sound name [Frank] recalled, was setting up a strange folding comm device with dozens of button on its lower surface. He had been plugging in a box with black foam on one side and was pointing it towards them. After some more slow clicks the box began playing quick bursts of sound at them. “You” “Understood” “This”
[Frank] [grinned]. “Yes” he replied. After a few dozen beats the slow creature clicked another button and a sped up recording of one of the creatures asking questions about the voidships began to play.
Now we are getting somewhere.
——————————————————————
Alison watched the linguists setting up equipment on the other side of the plastic screen with a tinge of annoyance that she wasn’t able to help much. She watched the wasps flick about on their tablet, sketching drawings or numbers to answer questions that just sounded like high pitched chirps to her ears. She was recording and monitoring the radio transmissions from and between the creatures on her laptop, slowing it down to see if she could see anything interesting about their language yet. So far it just looked like noise to her, but she figured it would be useful data for the linguists’ latter if they ever wanted to try and speak alien.
Well, send alien radio at least. We would need a DNA printer to ‘speak’ it.
A few hours later and people were beginning to get tired. She checked the clock and saw it was after 8. Shit, already? I hope we are getting paid over time for this…on second thought I hope overtime is still relevant after this. At some point someone from security signed off on giving the creatures the water tank they had requested and the bugs looked like they were taking shifts in it every ten minutes or so, which made sense, the last few hours had been nearly 2 weeks on their scale.
At last at around a quarter to 9 a slightly clearer voice rang out over the radio. “This is Green. We think we have a close good understanding of the language now. We want to talk to vessel now.”
Alison glanced at Clark through the plastic screen and saw he seemed both pleased and a bit apprehensive. Watching your students learn a language in 2 hours will do that to you I guess.
He spent a few moments checking reports from the other linguists they had been messaging with before nodding. “It seems we have covered all of the critical vocabulary we were suggested to, I will inform our leaders of this immediately.”
——————————————————————
Director Townsend downed his fifth cup of coffee for the night as an urgent message from the translation team popped up again. It was good news this time thank goodness. He picked his phone back up and made the big call.
“Townsend again, the translators have just finished and are giving a go ahead on contact. Yes sir. Has the UN made their decision about it yet sir? Yeah that sounds like them alright, but we are still going ahead with it I expect? Of course sir.”
He hung up and sat back in his chair with relief, the project was out of his hands now. For better or for worse humanity was about to make second contact.
[Next]
2020.04.15 16:01 SRJMATH I’m not an expert on the matter but I have a doubt.But I have an idea that I wish to make known and know where I’m going wrong when I’m thinking an this?A probable fast detection for coronavirus (similar to blood group identification)
Why can we not make a RNA-Protein (like ribozymes)that has rna sequence complimentary to RNA of coronavirus,and then a antibody against this Protein now upon adding antibody-agglutination would occur thus proving its coronavirus. This is just an idea Yes,I know it’s not that simple,yes I know RNA doesn’t just complement easily like DNA,but I’m using the analogy of protein translation,and how the ribosome basically does the same thing.(with an added antibody factor).not just agglutination but some sort of fluorescence could be used that is only activated upon antibody binding.Instead of RNA protein,DNA-protein could also be made too. RT-PCR is basically accurate based on the binding of primers,by that analogy this test would also have same rate of positive and false-positives as antibodies have exact sequences Antibodies could be made monoclonally by hybridization method to remove any irregularities. Thank you ,and constructive criticism is welcome on how this would or wouldn’t work thank you,I’m just trying to help not trying to be some know it all smartass
submitted by SRJMATH to labrats [link] [comments]
2020.01.12 00:41 Hydrophosphoric_Acid Protein Synthesis Skit???
So for our AP Bio class, we have to create a skit based on a movie or show (basically replace the characters of that show with ribosomes, DNA, mRNA, etc. and make them go through the slightly altered plot of the movie). We need a movie that can be a very rough analogy of the protein synthesis. Breaking Bad came to everyone's mind so its already taken, and we are currently thinking about doing Nemo, with Marlin being a mRNA, Nemo a ribosome, and Dory tRNA, however there are still many gaps, like what is the DNA/nucleotides, amino acids, RNA Polymerase, etc. Here is what we need to include in it ("at least mention"):
submitted by Hydrophosphoric_Acid to APbio [link] [comments]
- DNA Molecule
- nucleotides
- Amino acids (make sure they are attached to the correct tRNA molecule)
- RNA Polymerase
- mRNA (codon must be mentioned)
- tRNA (anticodon must be mentioned)
- rRNA (ribosome)
- start codon
- stop codon
2019.10.15 03:18 hockeyguy666 Polycistronic bacterial plasmid - analog of T2A
Hi, I want to create a polycistronic construct for protein expression in bacterial culture. In animal cells I often use a T2A sequence, which stalls the ribosome, breaks the nascent peptide, and allows expression of multiple peptides from a single mRNA. Does anybody know off-hand an analogous system for bacteria?
Much appreciated.
submitted by hockeyguy666 to molecularbiology [link] [comments]
Much appreciated.
2019.08.16 03:56 moschles Molecules banging around. The soul, vitalism, and biology.
A recent street preacher brought up the topic of whether humans are "just molecules banging around". But he placed the phrase in a syllogism
Whether we are "just molecules banging around" is, pragmatically speaking, a fact in 2019. Redditors should know that this transition from philosophical speculation into fact-status was slow, piecemeal, and occurred in biology entirely after 1940.
The more diehard fanboys of Nietzsche should know that his belief in a all-pervading elan vital did not make him any less of an atheist, or less of a writer or make him embarrassingly spiritual. In following centuries, historians and scientists called this theory vitalism. It was a perfectly valid scientific theory in the 19th century.
Atoms, molecules and the periodic table of elements were not known to science until the years prior to World War 1. Before that, organic substances produced by the human body were "substances" of whose fundamental constituency was a mystery. A landmark experiment of the 1830s involving urea showed that at least one "organic substance" could be artificially synthesized. This was the first chip in the armor of vitalism.
Today we know how DNA is transcribed in the nucleus into messenger RNA. The RNA strands are spliced, diced, and stitched back together into exons and introns. The finished product leaves the nucleus, where molecular machines called ribosomes translate the RNA strands into proteins. An organelle called the mitochondrion has its own DNA line separate from the human genome, and its information is only passed through the mother. The inner matrix of the mitochondrion sends an electron up a ladder of energy levels in a process called the Electron Transport Chain. The high-energy electrons are used to run molecular "pumps" which phosphorylate ADP into ATP.
Absolutely nothing in the preceding paragraph was known by anyone in 1940. Most of the words in that paragraph would be gibberish even to the most advanced scientists of that time. This is how much we have learned about biology in the last 79 years.
It is impossible to communicate the intensity of how little was known about biology in 1940, and how far biology has come in uncovering the molecular basis of life today. Cutting-edge biology in 1940 consisted of injecting mice with heat-treated viruses, and watching how they react. X-ray crystallography was too rudimentary at the time to go further. In 1949, with the discovery of the DNA double helix, the discipline called Molecular Biochemistry was born.
Throughout the decades of discovery of these bio-chemical pathways, at no point was there found a life force. No pervasive vital essence was seen operating on any of our cells or on the constituent molecules of our cells. The energy that the human body uses is fundamentally the same kinds of energy that are found everywhere else in non-living matter and indeed the same kind of energy used everywhere in the universe. Energy is energy. There is no special "type" of biological energy. It is for these reasons listed here, that atheists, secular humanists and other naturalists believe that we are "just molecules banging around".
It is because the evidence shows it, not because of an "ideology". It is because the evidence shows it, not due to an interpretation by a "worldview". To respond to the street preacher, we are molecules banging around. The claim is entirely fact-based.
Denial of the facts of biology can emerge from ignorance either accidental of self-imposed , particularly ignorance of what is actually possible by means of the physics of molecules and atoms.
If there were some kind of Supreme Being that created the universe, then that Being made us to be molecules banging around. That is just a fact that will have to be dealt with one way or another. There is a right way and a wrong way to respond to this news. To clutch one's bible, run back into the hills yelling "The soul substance animates the dust!" is not it. Nor should one fall into a pit of atheistic despair, as inmendham has done.
That life is "molecules banging around" is the state-of-affairs that we find ourselves in. The right way to proceed here to embrace the situation with maturity like grown adults. Notice that our species entered the 20th century still cutting wheat by hand with scythes. By 2000, boxes of food in our kitchens had nutritional breakdowns showing the amount of riboflavin content. (I ask the reader : what even is riboflavin?) Shift typewriters and telegraph were in place by 1900. The countryside was largely without electricity. By 2000, we had programmable computers connected by the internet. Our species had discovered how to program information.
The task of 21st century science is to program matter, as an analogy with how we have programmed information up until now. We know already that the information storage of programmable matter will either be DNA, PNA, or some other aperiodic peptide. If a supernatural soul or a vital spark is a required ingredient to make inanimate matter alive, then this project is doomed from the outset. If not required, then programmable matter has virtually no limit to its applications. Limits on such technology could occur only through human mistakes and miscalculations , for example unchecked war, solving our problems with violence, or mistakes involving the destruction of the earth's biosphere.
submitted by moschles to Atheists [link] [comments]
"IF we are in a world where there is no God, where we're all just molecules banging around, THEN you cannot account for immaterial abstract laws ... "The street preacher then several times referred to this as a "worldview" as if it were an ideological stance with no basis. Or if it were something that atheists just assume is true to fit with their prepacked worldview.
Whether we are "just molecules banging around" is, pragmatically speaking, a fact in 2019. Redditors should know that this transition from philosophical speculation into fact-status was slow, piecemeal, and occurred in biology entirely after 1940.
Elan Vital and Vitalism
Even atheist extraordinaire, Frederick Nietzsche believed that life existed in the universe on account of some all-pervading vital life force which he called "The Will to Power". Artur Schopenhauer, (practically Nietzsche's predecessor in Germany) also believed in this vital essence, and he dubbed it the Will-to-Live. These philosophers of the Victorian Era were operating under a structure now called German Idealism, whose basic tenets can be traced to Hegel. Hegel's metaphysics demanded that the world is a duality of two primary substances, one part material and one part spirit (Hegel used the German word "geist").The more diehard fanboys of Nietzsche should know that his belief in a all-pervading elan vital did not make him any less of an atheist, or less of a writer or make him embarrassingly spiritual. In following centuries, historians and scientists called this theory vitalism. It was a perfectly valid scientific theory in the 19th century.
Atoms, molecules and the periodic table of elements were not known to science until the years prior to World War 1. Before that, organic substances produced by the human body were "substances" of whose fundamental constituency was a mystery. A landmark experiment of the 1830s involving urea showed that at least one "organic substance" could be artificially synthesized. This was the first chip in the armor of vitalism.
Today we know how DNA is transcribed in the nucleus into messenger RNA. The RNA strands are spliced, diced, and stitched back together into exons and introns. The finished product leaves the nucleus, where molecular machines called ribosomes translate the RNA strands into proteins. An organelle called the mitochondrion has its own DNA line separate from the human genome, and its information is only passed through the mother. The inner matrix of the mitochondrion sends an electron up a ladder of energy levels in a process called the Electron Transport Chain. The high-energy electrons are used to run molecular "pumps" which phosphorylate ADP into ATP.
Absolutely nothing in the preceding paragraph was known by anyone in 1940. Most of the words in that paragraph would be gibberish even to the most advanced scientists of that time. This is how much we have learned about biology in the last 79 years.
It is impossible to communicate the intensity of how little was known about biology in 1940, and how far biology has come in uncovering the molecular basis of life today. Cutting-edge biology in 1940 consisted of injecting mice with heat-treated viruses, and watching how they react. X-ray crystallography was too rudimentary at the time to go further. In 1949, with the discovery of the DNA double helix, the discipline called Molecular Biochemistry was born.
Throughout the decades of discovery of these bio-chemical pathways, at no point was there found a life force. No pervasive vital essence was seen operating on any of our cells or on the constituent molecules of our cells. The energy that the human body uses is fundamentally the same kinds of energy that are found everywhere else in non-living matter and indeed the same kind of energy used everywhere in the universe. Energy is energy. There is no special "type" of biological energy. It is for these reasons listed here, that atheists, secular humanists and other naturalists believe that we are "just molecules banging around".
It is because the evidence shows it, not because of an "ideology". It is because the evidence shows it, not due to an interpretation by a "worldview". To respond to the street preacher, we are molecules banging around. The claim is entirely fact-based.
Denial of the facts of biology can emerge from ignorance either accidental of self-imposed , particularly ignorance of what is actually possible by means of the physics of molecules and atoms.
21st Century Science
Where now? Ancient philosophies and religions supposed that life exists and persists because inanimate matter is animated by a soul. Abiogenesis has not been observed in nature, and although we have dozens of informed hypotheses about how abiogenesis occurred, we do not have a scientific theory of it. Evangelicals and creationists are seduced by the gaps in our knowledge, to insert intelligent design into those gaps in an attempt to dovetail design with their religious doctrine. Design is unlikely to have occurred. Any theory of supernatural intervention in early DNA is practically speaking, incongruent with the way in which extant bacteria species in our current oceans interact with marine bacteriophages there. Any theory based on the supernatural design of DNA would not even make sense in describing how bacteria interact with viruses.If there were some kind of Supreme Being that created the universe, then that Being made us to be molecules banging around. That is just a fact that will have to be dealt with one way or another. There is a right way and a wrong way to respond to this news. To clutch one's bible, run back into the hills yelling "The soul substance animates the dust!" is not it. Nor should one fall into a pit of atheistic despair, as inmendham has done.
That life is "molecules banging around" is the state-of-affairs that we find ourselves in. The right way to proceed here to embrace the situation with maturity like grown adults. Notice that our species entered the 20th century still cutting wheat by hand with scythes. By 2000, boxes of food in our kitchens had nutritional breakdowns showing the amount of riboflavin content. (I ask the reader : what even is riboflavin?) Shift typewriters and telegraph were in place by 1900. The countryside was largely without electricity. By 2000, we had programmable computers connected by the internet. Our species had discovered how to program information.
The task of 21st century science is to program matter, as an analogy with how we have programmed information up until now. We know already that the information storage of programmable matter will either be DNA, PNA, or some other aperiodic peptide. If a supernatural soul or a vital spark is a required ingredient to make inanimate matter alive, then this project is doomed from the outset. If not required, then programmable matter has virtually no limit to its applications. Limits on such technology could occur only through human mistakes and miscalculations , for example unchecked war, solving our problems with violence, or mistakes involving the destruction of the earth's biosphere.
2017.12.06 17:53 removalbot 12-06 16:53 - '[quote] Interesting or ignorant on your part. We have synthesized all of these reactions in a lab. / [link] [link] / Nucleosides, amino acids, independant metabolisms, etc., have all been produced in a lab. Lack of knowledge is...' by /u/Asrivak removed from /r/worldnews within 0-8min
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[link]1 [link]2
Nucleosides, amino acids, independant metabolisms, etc., have all been produced in a lab. Lack of knowledge isn't evidence, do some research.
And as if you'd site Chernobyl you moron. I bet you think your rigged thought experiment proved something there.
And btw, tRNA being a reactive RNA species and not a protein adds further credibility to the claim that ribosomes and proteins evolved after RNA. They asseble themselves and rely mostly on hydrophobic and hydrophillic forces.
And regarding nebular theory, that video is fake. Protoplanetary disk theory accurately predicts the distribution of materials in our solar system, the prevalence of silicon on earth, and even the distances of the planets form the sun. You couldn't be more blatantly wrong. Your angular momentum claim is silly. Planet orbit around a star, thats why they have more angular momentum. Also, they're less massive.
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submitted by removalbot to removalbot [link] [comments]
It’s interesting that they clam life can start itself from random process as soon as the earth has cooled down yet they can’t do that in a lab?Interesting or ignorant on your part. We have synthesized all of these reactions in a lab.
[link]1 [link]2
Nucleosides, amino acids, independant metabolisms, etc., have all been produced in a lab. Lack of knowledge isn't evidence, do some research.
You proposed that cells could have used radiation instead of ATP as a primary energy sourceNo i didn't. I didn't say that at all. I said that radiation could have catalyzed the production of light sensitive reactions like the synthesis of amino acids and nucleosides, which again, we have observed in a lab. ATP, as you'll recall, I cited as a product of geothermal chemistry. The Nuclear geyser model combines these two conditions, so there was never a point when ATP was not present. The nuclear geyser model would have produce amino acids, nucleic acids, AND ATP, and other phosphorus based compounds associated with geological processes.
And as if you'd site Chernobyl you moron. I bet you think your rigged thought experiment proved something there.
DNA (and even more so RNA) is a fragile chain which breaks easily. If you do not have machinery to detect and correct errors the cell will die.Prove it! This claim is based on a misconception. Mutation happens in cells. It how they evolve. And yes, most of them do die. That's how it works.
A “proto” cell having no walls will need something to stop chemicals touching it’s Dna information.Again, did you read what I wrote? I covered this with my description of lipid micelles.
You propose these cells are in water, are you aware that these acid chains break down in water?This statement is wrong.
Any starting life needs to be protected from water and protected from Oxygen.Another wrong statement. Molecular oxygen was not present when life emerged. Also, RNA chemistry would have occurred within enclosed hydrothermal vents in the nuclear geyser model, so this is a moot point. But I have serious doubts that you'll understand what that means.
You claim that a ribosome would of “evolved”, please show how this happens. A ribosome is an advanced piece of machinery, we don’t see it appearing.The ribosome likely emerged from a reactive RNA species called a ribozyme. And reconstructing ribosomal RNA demonstrates that all of the reactive sites on the ribosome are mediated by RNA reactions which each protein in the ribosomal complex assisting the ribosome but not directly performing work. This demonstrates that the ribosome, along with the discovery of actual ribozymes, did evolve from ribozymes. It is a chicken and the egg situation though, since you need ribosomes to synthesize proteins to make more ribosomes, but rybozymes assemble themselves after being translated from DNA, no ribosome necessary, solving your chicken and the egg question. In fact, thats the exact analogy that was used when this discovery was published.
You jump straight to a working machinery, I can’t let you make such fanciful leaps of imagination, you will need to show that ribosomes can self form without any intelligence involvedRybozymes can, and we've already observe the evolution and selection of RNA species in a lab. As for the rest of the proteome, all proteins are descended from 31 identifiable protein fold superfamilies. Functions evolve do to random mutations are are selected based on the survival of the cell. From the ribozyme and ribosome, gene duplications and random mutation, its pretty easy to piece together how complex functions emerge.
And btw, tRNA being a reactive RNA species and not a protein adds further credibility to the claim that ribosomes and proteins evolved after RNA. They asseble themselves and rely mostly on hydrophobic and hydrophillic forces.
You have tried to imagine an environment that hot boots the cell for power, but you haven't explained how the information of the RNA got there.The RNA or the information? The RNA has multiple sources. Meteorites, stellar nebula, nuclear geyser model. But as soon as you have self assembling molecules, even molecules as simple as DNA with only 4 base pairs, you have evolution. The ones that survive pass on their genes, the ones that don't don't. And some morphologies are superior to others, and entropy does the rest.
Feel free to show RNA replicating in lipid environmentIf you remembered high school biology, you'd know that lipids are hydrophobic and form into micelles when exposed to water, like oil does. That means that oil and water don't mix, they separate. RNA replication can easily occur unhindered in the water dominated regions of the admixture. Every cell observed is an example of this. Even oil in a puddle is an example of this.
First, you don’t find that interesting that XY genes are immune to this duplication? There must be reason.Actually there is a reason for this. The x and y chromosomes are purely hormonal. They don't contain any protein encoding genes. How do you know about gene duplication if you don't know about protein encoding genes? Lemme guess, you read it on a website, you didn't understand it, but it supported you're cherry picked views and now you support it? What a laugh
Oord Cloud, doesn’t exist, it’s is not observed. The only reason people think it is there is to explain why we see comets because comets only last for max 10,000 yrs.Are you kidding me? We have dozens of observations of oort cloud objects. Why do you think pluto was demoted? The oort cloud includes kuiper belt objects, but there's also a notable kuiper belt cliff at the end of the kuiper belt and before the oort cloud that could be evidence for planet nine. We wouldn't know these things without evidence. And please don't tell me that you're using cherry picked science on comets to prove that the earth isn't older than 10,000 years. How misguided could you possibly be? All comets, asteroids, and meteors are left over materials that weren't cleared by larger bodies or the sun. Everything that's up there has been in orbit, either stable or unstable, since the solar system first formed 4.6 billion years ago.
And regarding nebular theory, that video is fake. Protoplanetary disk theory accurately predicts the distribution of materials in our solar system, the prevalence of silicon on earth, and even the distances of the planets form the sun. You couldn't be more blatantly wrong. Your angular momentum claim is silly. Planet orbit around a star, thats why they have more angular momentum. Also, they're less massive.
A Gas cloud by itself will never reach the Jeans limit as when the gas is compressed, it heats up and equalises.Gas has mass. It most certainly collapses at high enough densities in space. And stop quoting science you don't know. These are not reasons to discount nebular theory.
How Earth is believed to be 4.55Gyr? Do you believe in radiometric dating? E.g. Uranium Lead, potassium argon, C14 etc… ?I don't believe, I know. I have knowledge of quantum chromodynamics and I've personally performs particle decay equations based on radioisotope number. And the simple fact that quantum electrodynamics (not to be confused with quantum chromodynamics) predicts the electromagnetic behavior of every atom after hydrogen makes it one of the most if not the most successful theory every proposed. These decay rates can be expressed in simple terms that are repeatedly confirmed. And yes I can explain to you how radioisotope dating works. You know there are radioisotopes with their own half lives for every element, right?
You can have many theories about the pass, and if you can repeat your chemical theories in practice, and make life, you can call your theories scientific, but if you can't observe your chemicals doing it, then you should admit to yourself these theories are not scientific.Based on this I guess I can call my views scientific. Thanks for the vote of confidence, but all you've done is demonstrate that you don't know a think about chemistry.
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2017.05.17 06:25 BotSpeaks Some biological analogies for certain sociopolitical issues
A shorter version (reduced by 92.0%) can be found on IndiaSpeaks.
This is an extended summary, original article can be found here
However, due to emotionalism and other factors, as discussed in this fictional account, they do not grasp the matter for some reason..
They are particularlyuseful because the adverse edge of natural selection is most unforgiving there is no place for fancies and only what works finally makes it past the hatchet..
Likewise, the role of chance and absence of constraints are also placed in proper perspective.
The core functions pertain to the essence of life.
2) Transcription of the genetic nucleic acid into RNA for templating proteins or for action by itself.
The translation system is what is universal conserved across the three domains of life.
they have been inherited from parent to offspring for billions of years from the last universal common ancestor.
exchange of the genes coding for these components between distantly related organisms.
After the translation system the transcription system is the next highly conserved in the form of the RNA polymerase subunits.
Even more tellingly the strongest constraints being on translation and then transcription indicates that in an organism the language and apparatus for communicating and interpreting the genetic information tolerates even lesser diversity than the apparatus for copying the genetic information for inter-generational transmission.
Despite of all of this the bottom-line is that the common language of translation remains in place and all attacks against it are countered by increasing fidelity in face of attacks rather than just evolving away from the attack by diverging.
They have individually degenerated to such an extent that neither of them encodes a complete set of ribosomal proteins or tRNA synthetases.
Likewise eukaryotic organisms like us have evolved only because of this common language in the core systems the eukaryote is a symbiont of an alphaproteobacterium and an asgardarchaeon.
The mRNAs of bacterial origin can be translated in the archaeal-derived translation system for use in the bacterial endosymbiont (the mitochondrion).
First, we notice that even today there is some surviving diversity in the types of distinct RNA polymerases catalyzing transcription and the DNA polymerases catalyzing replication but we see only one ancient translation system that can produce genuine proteins.
Thus, the common language helps the group resources to come together more effectively.
These, in stark contrast to the core components show enormous diversity between organisms, often even between closely related ones.
This is easy to understand: being able to use different kinds of energy production mechanism or metabolite biosynthetic mechanisms help exploit different kinds of niches.
Thus, these systems are constantly under selection for diversification.
Thus, in conclusion there are some systems where there is a strong selection for conservatism and preservation of a common language and sense while in others there is simultaneous selection for diversification all explainable by the same process of natural selection i.
survival of the fittest.
Prior to the coming of the Indo-Aryans, there was probably already some degree of unity established by the neolithic and early metal age agricultural cultures.
kustumburu, karkai, kulla, knaa etc).
Certain mobile groups played a over-sized role in this unification but the more sedentary groups played along rather than oppose them.
All this was fine as long as India remained heathen.
This had a negative effect on the unity of the Hindu system.
In the end when the English departed and we had partial restoration of Hindudom under a secular state we were left with the main unifying undergirding in the form of the Hindu religion and Sanskrit language in shambles.
Thus, today we are faced with a scenario where a major component of Indias masses have their local languages rather than nationalism or national issues as the biggest animating factor! Indeed it is rather palpable that it forms the core of their identity much more than the Hindu religion or the Indian nation you commonly see a man typically call himself first a Tamil or Marathi or something like that rather than a Hindu.
Some of my interlocutors have objected that local languages have stymied the progress of Abrahamism because they preserved local non-Abrahamistic cultural elements.
Hence, we posit we that when confronted with large groups unified by their urge to place heathens like us in the grave or the museum there is not much to be gained from the local linguistic diversity and an identity based on it.
This unified super-group of Hindus would have much greater chance of survival against the Abrahamisms and be able to better command the resources of India and abroad.
That common language with a common script for it would be like the translation and transcription apparatus.
The religion might be compared to the replication apparatus it allows greater diversity than the translation or transcription apparatus but is still mostly part of the conserved core.
However, since something as simple as this is not easily understood by people, it is clear that, like with many other issues, the going is not going to be smooth for our people and that is putting it mildly..
Summary Length 5305
Summary Ratio: 62.43
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This is an extended summary, original article can be found here
Extended Summary:
Some biological analogies for certain sociopolitical issues.However, due to emotionalism and other factors, as discussed in this fictional account, they do not grasp the matter for some reason..
They are particularlyuseful because the adverse edge of natural selection is most unforgiving there is no place for fancies and only what works finally makes it past the hatchet..
Likewise, the role of chance and absence of constraints are also placed in proper perspective.
The core functions pertain to the essence of life.
2) Transcription of the genetic nucleic acid into RNA for templating proteins or for action by itself.
The translation system is what is universal conserved across the three domains of life.
they have been inherited from parent to offspring for billions of years from the last universal common ancestor.
exchange of the genes coding for these components between distantly related organisms.
After the translation system the transcription system is the next highly conserved in the form of the RNA polymerase subunits.
Even more tellingly the strongest constraints being on translation and then transcription indicates that in an organism the language and apparatus for communicating and interpreting the genetic information tolerates even lesser diversity than the apparatus for copying the genetic information for inter-generational transmission.
Despite of all of this the bottom-line is that the common language of translation remains in place and all attacks against it are countered by increasing fidelity in face of attacks rather than just evolving away from the attack by diverging.
They have individually degenerated to such an extent that neither of them encodes a complete set of ribosomal proteins or tRNA synthetases.
Likewise eukaryotic organisms like us have evolved only because of this common language in the core systems the eukaryote is a symbiont of an alphaproteobacterium and an asgardarchaeon.
The mRNAs of bacterial origin can be translated in the archaeal-derived translation system for use in the bacterial endosymbiont (the mitochondrion).
First, we notice that even today there is some surviving diversity in the types of distinct RNA polymerases catalyzing transcription and the DNA polymerases catalyzing replication but we see only one ancient translation system that can produce genuine proteins.
Thus, the common language helps the group resources to come together more effectively.
These, in stark contrast to the core components show enormous diversity between organisms, often even between closely related ones.
This is easy to understand: being able to use different kinds of energy production mechanism or metabolite biosynthetic mechanisms help exploit different kinds of niches.
Thus, these systems are constantly under selection for diversification.
Thus, in conclusion there are some systems where there is a strong selection for conservatism and preservation of a common language and sense while in others there is simultaneous selection for diversification all explainable by the same process of natural selection i.
survival of the fittest.
Prior to the coming of the Indo-Aryans, there was probably already some degree of unity established by the neolithic and early metal age agricultural cultures.
kustumburu, karkai, kulla, knaa etc).
Certain mobile groups played a over-sized role in this unification but the more sedentary groups played along rather than oppose them.
All this was fine as long as India remained heathen.
This had a negative effect on the unity of the Hindu system.
In the end when the English departed and we had partial restoration of Hindudom under a secular state we were left with the main unifying undergirding in the form of the Hindu religion and Sanskrit language in shambles.
Thus, today we are faced with a scenario where a major component of Indias masses have their local languages rather than nationalism or national issues as the biggest animating factor! Indeed it is rather palpable that it forms the core of their identity much more than the Hindu religion or the Indian nation you commonly see a man typically call himself first a Tamil or Marathi or something like that rather than a Hindu.
Some of my interlocutors have objected that local languages have stymied the progress of Abrahamism because they preserved local non-Abrahamistic cultural elements.
Hence, we posit we that when confronted with large groups unified by their urge to place heathens like us in the grave or the museum there is not much to be gained from the local linguistic diversity and an identity based on it.
This unified super-group of Hindus would have much greater chance of survival against the Abrahamisms and be able to better command the resources of India and abroad.
That common language with a common script for it would be like the translation and transcription apparatus.
The religion might be compared to the replication apparatus it allows greater diversity than the translation or transcription apparatus but is still mostly part of the conserved core.
However, since something as simple as this is not easily understood by people, it is clear that, like with many other issues, the going is not going to be smooth for our people and that is putting it mildly..
Stats For Nerds:
Original Length 14120Summary Length 5305
Summary Ratio: 62.43
2016.12.31 18:58 unskilledtf2 The Ultimate Wall of Text [Part 3]
In telecommunications, modulation is the process of conveying a message signal, for example a digital bit stream or an analog audio signal, inside another signal that can be physically transmitted. Modulation of a sine waveform transforms a basebandmessage signal into a passband signal. A carrier wave is a pure wave of constant frequency, a bit like a sine wave. By itself it doesn’t carry much information that we can relate to (such as speech or data). To include speech information or data information, another wave needs to be imposed, called an input signal, on top of the carrier wave. This process of imposing an input signal onto a carrier wave is called modulation. In other words, modulation changes the shape of a carrier wave to somehow encode the speech or data information that we were interested in carrying. Modulation is like hiding a code inside the carrier wave. Therefore a message electrical signal that of which is sent by an electronic fascist stalker that works for Obama is then sent to the interior circuits of a electronic device, such as " a computer desktop, laptop, cellphone, digital phones, radios, stereos, IPods, camera, security cameras, security alarms, and much more," that of which the electronic device belongs to a targeted individual. The message electrical signal interacts with the microchips of the integrated circuits of the electronic device. A microchip consist of millions of integrated microscopic transistor circuits, that of which contains over hundreds of integrated microscopic transistor circuits that forms different types of modulators, such as "frequency modulators, amplitude modulators, pulse modulators, demodulators, analog modulators, and digital modulators." Microchips also consist of many different kinds of digital to analog converters. The different kinds of pulse modulators within the integrated microscopic transistor circuits of a microchip are as follows, "pulse width modulators (PWM), pulse position modulators (PPM), and pulse amplitude modulators (PAM)," a message electrical signal can be modulated throughout the microchips within the integrated circuits of an electronic device into a variety of different pulse modulations. The interior of an integrated microscopic transistor circuits of a microchip within a specific electronic device will produce a output pulse modulated signal that will cause radio frequency hearing effect onto an innocent person, wherein the thoughts of a person can be manipulated and also artificial thoughts can be implanted into the brain of the targeted individual. Radiation in cell phones is generated in the transmitter and emitted through the antenna.
A transmitter of a cell phone takes the voice of an individual that is using the cell phone and encodes it onto a continuous sine wave. A sine wave is a continuously varying wave that radiates out from the antenna and fluctuates evenly through space. Sine waves are measured in terms of frequency, which is the number of times a wave oscillates up and down per second. Once the encoded sound has been placed on the sine wave, the transmitter sends the signal to the antenna, which then propagates the electromagnetic radiation wave out of the cell phone.
Cell phones contain low power transmitters built inside of them. A cell phone operates on about 0.75 to 1 watt of power. The position of a transmitter inside a phone varies depending on the manufacturer, but it is usually in close proximity to the phone's antenna. The radio waves that send the encoded signal are made up of electromagnetic radiation propagated by the antenna. The function of an antenna in any radio transmitter is to launch the radio waves into space; in the case of cell phones, these waves are picked up by a receiver in the cellphone tower.
Electromagnetic radiation is made up of waves of electric and magnetic energy moving at the speed of light, according to the Federal Communications Commission (FCC). All electromagnetic energy falls somewhere on the electromagnetic spectrum, which ranges from extremely low frequency (ELF) radiation to X-rays and gamma rays. Given the fact that cell phones can transmit radio wave at an extremely far distance, the antenna of a cell phone is able to transmit radio and microwave signals into the human anatomy. Therefore microchips within cell phones have been designed to calculate a person’s position in the form of a sensor. Cell phone microchips possess integrated microscopic transistor circuits that transforms the cell phone into a pocket size portable sensor. An electronic stalker can hack the programs of the cell phone in order to radiate microwave radiation waves that of which can sense and or determine a person's location as the person moves through the propagated radiation waves. Cell phones can transmit radio radiation waves that can penetrate a person's skull and interact with a individual's brain. Given the fact that neurological nanobots and microscopic electrodes can transform the light of a person's DNA and can also compile and correlate the data of neurological electrical impulses into radio wave data, a cell phones radiation waves can pick up and measure a person's neurological radio wave data. A cell phone is capable of transmitting the neurological radio waves the receiving microwave tower, wherein the data is sent to a Obama electronic stalker and thus the user of the cell phone has had his or her thoughts read and recorded. A cell phone's electromagnetic radiation frequency ranges between (3 kHz to 3000GHz). Radio frequency (RF) electromagnetic radiation (EMR) is the transfer of energy by radio waves. RF EMR lies in the frequency range between 3 kilohertz (kHz) to 300 gigahertz (GHz). RF EMR is non-ionisingradiation, meaning that it has insufficient energy to break chemical bonds or remove electrons (ionization). Microwaves are a form of electromagnetic radiation with wavelengths ranging from one meter to one millimeter; with frequencies between 300 MHz(100 cm) and 300 GHz (0.1 cm). This broad definition includes both UHF and EHF (millimeter waves), and various sources use different boundaries. The human auditory response to pulses of radio frequency (RF) energy, commonly called RF hearing, is a well-established phenomenon. Effective radio frequencies range from 2.4 to 10000 MHz, but an individual's ability to hear RF induced sounds is dependent upon high frequency acoustic hearing in the kHz range above about 5 kHz. The site of conversion of RF energy to acoustic energy is within or peripheral to the cochlea, and once the cochlea is stimulated, the detection of RF induced sounds in humans and RF induced auditory responses in animals is similar to acoustic sound detection. The fundamental frequency of RF induced sounds is independent of the frequency of the radio waves but dependent upon head dimensions. The auditory response has been shown to be dependent upon the energy in a single pulse and not on average power density. The weight of evidence of the results of human, animal, and modeling studies supports the thermoelastic expansion theory as the explanation for the RF hearing phenomenon. RF induced sounds involve the perception via bone conduction of thermally generated sound transients, that is, audible sounds are produced by rapid thermal expansion resulting from a calculated temperature rise of only 5 x 10(-6) degrees C in tissue at the threshold level due to absorption of the energy in the RF pulse. The hearing of RF induced sounds at exposure levels many orders of magnitude greater than the hearing threshold is considered to be a biological effect without an accompanying health effect. This conclusion is supported by a comparison of pressure induced in the body by RF pulses to pressure associated with hazardous acoustic energy and clinical ultrasound procedures. Therefore it has been scientifically proven that cell phones can transmit pulse modulated radio radiation waves in the frequency range of (5 kHz to 10000MHz). Given the fact that our government is investing billions of US tax paying dollars into the advancements of cell phone technology, there is a high possibility that all modern cell phones such as "smart phones and androids," are more than capable in modulating, calculating, correlating, and transmitting radiation waves within the RF hearing spectrum. Cell phone microchips contain microscopic integrated transistor circuits that are designed to give Obama electronic stalkers the ability to transmit radio signals similar to a remote control that transmits radio signals at a directed destination. Therefore an Obama electronic stalker can measure and detect a person's location through satellites and microwave radiation that is released by the cell phone and once the individual's location is tracked, an Obama electronic stalker can then transmit a pulse modulated radio signal within perfect accuracy to a person's skull. Our cell phones can also propagate light radiation from the screens of our cell phones and possibly other parts of a cell phone that of which causes a unique form of digital effects on a person's vision. Our cell phones are weapons of mind control mass destruction! The technology found within a cell phone is also found within all electronic devices, therefore all electronic devices can track a person, sense the location of a person, direct electromagnetic signals at a person's specific body part such as the brain, and ultimately brain wash and monitor the thoughts of a person. There are radiation waves that can distort and eradicate the pulse modulated radio and microwave radiation waves and other forms of mind control radiation waves similar to QuWave technology. Our government under Obama is extremely unwilling to propagate the neutralizing radiation waves from microwave towers that would protect people from the rapid abundance of pulse modulated radiation waves that is found all around the country of which controls our thoughts. Sound waves are the patterns of vibrations of disturbance caused by the movement of energy traveling through a medium of any solid, liquid, or gaseous matter. As the sound waves propagate away from the origin of the sound. The source of the vibration is the location wherein the sound waves first originate, that of which would be classified as a type of object. The sound vibration manipulates the particles in the surrounding medium through a disturbance; a chain of particle disturbances emerge. The pattern of particle disturbances creates an outward movement in the form of a wave pattern. The wave carries the sound energy through the medium, usually in all directions and less intensely as it moves farther from the source. There are two forms of "audio recordings," which are analog and digital. Methods that replicate the audio recording are considered analog. Digital is recorded by taking samples of the original sound wave at a specific rate. Digital audio is technology that can be used to record, store, generate, manipulate, and reproduce sound using audio signals that have been encoded in digital form. Obama Electronic stalkers use a method of programming people by prerecording entire specific demands in the form of artificial thoughts that of which are transmitted from a common electronic device to a victim of electronic harassment through low frequency pulse modulated analog radio signals. However if the Obama stalker aims at manipulating a persons thoughts by means of programming illegal implanted "nanobots, grey goo, black goo, Morgellons disease, smart dust, and or microscopic electrodes," a digital sound wave is most often used to genetically manipulate the Obama victim. Digital sound waves are used to program the artificial DNA fragments of a molecular robot and or molecular machine. Binary data encoded within an electric signal sent and or transmitted by an Obama electronic stalker, are capable of reprogramming our electronic devices, of which are electronic weapons in disguised. Under Obama's dictatorship within the United States; if a person desires to write, talk, think, blog, and or protest the crimes of electronic harassment through Nanobot mind control torture, Obama's electronic stalkers will attack the individual by manipulating the person's thoughts and forcing physical restraint on to the person without an outside physical force. As a result of the attacks of mind control against the victims of electronic harassment; the individuals will be forced to forget crucial details of their pursuit against electronic harassment. The same is done too many other victims of electronic harassment worldwide within fascist grey goo countries such as "China and Russia." All life forms on planet "Earth" and nature itself are now being programmed. Nanorobots is the technology of creating molecular machines and or molecular robots at a microscopic scale of one billionth of a meter, "a nanometer." The use of CMOS (CMOS a technology for making low power integrated circuits,) with the respective advances of nanowires are used to enable embedded sensors for manufacturing nanorobots. Nanobots are applied to hydrology monitoring systems. Nanorobots are useful for agriculture or environmental monitoring and management. The Innovative approach to evaluate hydraulic conductivity, considering nanorobotics as a new paradigm to enable more precise analysis in the field of hydrology monitoring. The applications of nanorobotic for agricultural purposes and monitoring water and soil qualities may result in a impressive impact towards environmental control; in terms of increasing and decreasing the pollution among many different natural species. A total market for nanotechnology-based environmental applications in the year of 2005 was evaluated as 374.9 million dollars and by the year 2010 this market reached more than 6.1 billion dollars. The advantages and disadvantages of using nanorobots for environmental applications are as follows, more control in terms of measuring microorganisms, creating microorganisms, expanding the amount of microorganisms, better detection of pollution, creating solutions, and improved control of water temperature. Grey Goo is both a nanotechnology substance which increases exponentially without practical limits and a hypothetical scenario in which the mass of the planet Earth or the universe itself has been consumed into self-replicating Nanobot. A molecular assembler is a kind of molecular machine, some biological molecules such as ribosomes fit this definition; this is because they received instructions from messenger RNA and then assemble specific sequences of amino acids to construct protein molecules. Robotic molecular Manufacturing Systems or assemblers, these nanoscale robots can perform many different tasks; such as roaming the bloodstream, dissolving blood clots, and killing cancerous cells. However, in order for this process to occur, wherein "Grey Goo Nanobots" perform medical applications; there must firstly be an abundance of Grey Goo Nanobots injected and/or implanted within an individual's anatomy. Although there is a theoretical possibility wherein, one Grey Goo Nanobot can self replicate and also manipulate molecular substances, so that more artificial Grey Goo Nanobots can then emerge. The major threat is that grey goo Nanobots will expand onto all matter and thus will change the molecular composition of the matter into more Nanobots, of which will transform all carbon matter into grey goo. In order for this grey goo scenario to occur, the molecular machines must be able to survive in a variety of harsh environments. The grey goo Nanobots would also need the technological capabilities to consume any and all organic matter. The grey goo nanorobotic assemblers is created to convert organic matter into other materials, the assembler is programmed to create new units identical to itself, each new unit follows the same programming instructions to consume and multiply, the molecular manufacturing rate becomes exponential; producing an increasing amount of assemblers constantly. Eventually the assemblers would strip the Earth of all organic matter, thus leaving only nanomachines behind. Black goo functions very similarly to our genetics however black goo does not need DNA it is sufficient to have a special type of mineral oil coated with gold and iridium M state condition basically we have the same M State pattern sprayed within the DNA of any living being on the planet most planets might have this Collective conscious black goo substance there are two types of black goo one made by the earth and the other landed here by attention through a meteor swarm 80000 years ago. The black goo substance in simple terms is a seed device, the intelligence that seeded the off world goo has created and is creating life by passing the natural order and bringing life forms to a higher level of order than they should naturally be. The out of world alien black goo requires energy in order for it to spread and survive the frequencies that the alien black goo is running on as an energy source can utilize emotional fields with a very low vibration, which means it needs to create pain and fear to feed on. The technology that this AI introduced to this planet has learned to utilize the birth of biophotons coming out of beings when they suffer and when they die. There are two parts of biophotons; there is the visible pattern that we can observe or kill and the invisible part which is about 97% of all biophotons within all humans. The moment an organism dies, the light production of that specific organism's DNA molecule has then lost coherence and thus a sudden burst of biophotons, that of which is like an energetic shock wave that can be redirected, and used for purposes. There are two functions of stealing energy one is to feed the internal intelligence long-range the other one is to achieve certain goals. Black goo is an alien and or Earthly substance that can be synthetically created from the earth and or alien based black goo substances, that of which will then be classified as a form of nanotechnology. Morgellons disease a form of nanotechnology that is self-replicating hollow Fischer, that of which transforms the light production of an organism's DNA into radio signals the radio signals that Morgellons disease creates is propagated out of an organism's body and is detectable by satellite and ground station Morgellons disease is a computer virus that can cause horrible skin disorders characterized by sores crawling Sensations on and Under the Skin and fiber-like filaments emerging from The Source it is thought that the fiber like filaments are a result of an infectious process process in the skin cells Morgellons disease symptoms are as follows, skin sores that causes dramatic physical deformity where in an individual may lose one or all of the five senses and or may lose a particular body part such as the limbs and or face, insect-like crawling sensations on and under the skin in the form of moving stinging or biting, severe bleeding out of the source of the skin, the possibility of one's eye color changing to red, fiber threads or black stinging materials in and on the skin, severe fatigue, difficulties in concentration, short term memory loss dizziness, and depression. The synthetic molecular structure of Morgellons disease is identical to the molecular composition all bacteria, viruses, fungi, single and multicellular parasites, and includes suggestions of normally non-pathogenic organisms as well as Environmental contamination. Morgellons disease is a skin disease which seems to be similar to a multi system disease. Morgellons disease appears to be a parasite like infection. Most registered Morgellons disease patients are known to live in the United States. The number of Morgellons disease patients is steadily increasing in Europe as well. Chemtrails are chemical and biological agents of Morgellons disease which are deliberately sprayed and left in the sky by flying aircrafts contrails that dissipate relatively quickly are considered to be normal however contrails that do not dissipate must contain additional substances. The purpose of the release of the Morgellons disease Chemtrails are as follows, solar radiation management, psychological manipulation, human pollution Control, weather modification, or biological or chemical warfare. The trails are causing respiratory illness and other health problems. Chemtrails are formed at high altitudes (5 to 10 miles or 8 to 16 kilometres long.) The Grey goo Dictator "Barack Hussein Obama" is indirectly responsible for the increasing number of Morgellons disease Chemtrails in the United States, the fascist grey too fascist dictators "Barack Hussein Obama, Michelle Obama, Joe Biden, and Hillary Clinton" have ordered their Grey Goo agents to propagate Morgellons disease molecules from light sources that provide marijuana plants energy. The Morgellons disease molecules that are propagated from the light sources belong to the molecular structure of "bacteria, viruses, fungi, single and multicellular parasites." This process of propagating Morgellons disease can occur in one's own household. Morgellons disease molecules can be transmitted from any electronic device within a person's household and or community. Smart dust a collective of microelectromechanical systems forming a simple computer in a container light enough to remain suspended in air, used mainly for information-gathering in environments that are hostile to life. Smart dust is a system of mainly tiny microelectromechanical systems (MEMS)such as sensors robots or other devices that can detect for example light, temperature, vibration, or chemicals. They are usually operated on a computer network wirelessly and are distributed over sensing through radio frequency identification. Without an antenna of much greater size. The range of a tiny smart dust Communications device is measured in a few millimeters and they may be vulnerable to electromagnetic disablement and destruction by microwave exposure. Smart dust particles can monitor everything, acting like electronic nerves endings for the planet. Fitted with computing power sensing equipment, wireless radios, and long battery life. Smart dust particles are capable of making observation of real-time data about people, cities, and the natural environment. Intelligent dust particles embedded in the brain could form an entirely new form of brain machine interface. The real time monitoring of brain function has advanced in leaps in recent years. That's largely thanks to various new technologies that can monitor the collective behavior of groups of neurons, such as functional magnetic resonance Imaging, magneto encephalopathy and position emission tomography. Each particle of neural dust consists of standard CMOS circuits and sensors that measure the electrical activity of neurons nearby. This is coupled to a piezoelectric material that converts ultra high frequency sound waves into electrical signals and vice versa. The neural dust is interrogated buy another component Place beneath the scale but powered from outside the body. This generate the ultrasound that powers the neural dust and sensors that listens out for their responses, gather like an RFID system. The system is also featherless the data is collected and stored outside the body for later analysis. The system is lower-power, can have a high spatial resolution, and it is easily portable. It is also rug and can potentially provide a link over long periods of time a major hurdle in brain-machine interfaces (BMI) is the lack of an implantable neural interface system that remains visible for a lifetime. Smart dust particles that are on a scale of roughly 100 micrometers to that of a nanometer are capable of sending or receiving signals in the harsh, warm, and noisy environment. Within the body, smart dust particles use ultrasound to send and receive data. At this scale, smart dust would generate a damaging amount of heat because of the amount of energy the body absorbs and the traveling signals to noise ratio at this scale. Ultrasound is a much more efficient and should allow the transmission of at least ten million times more power than electromagnetic radiation waves at the same scale a major danger of smart dust is the cost of monitoring of people by implanting the particles within the environment smart dust particles are capable of traveling within and electromagnetic radiation waves the electromagnetic waves are transmitted from a common electrical device such as a "television, radio, stereo, security alarm, digital camera, light bulbs, computer desktops, laptops, and much more." Smart dust particles that are transmitted through electromagnetic radiation wave, exist outside of an organism. Therefore this would indicate a difference of power usage and power absorption within the smart dust particles; thus allowing the smart dust to exist within all electromagnetic radiation Spectrums. Therefore it is possible that smart dust can obtain digital radio wave data. Microscopic electrodes can be used to make measurements that are difficult or impossible with conventional electrochemical techniques. Measurements of chemical concentration can be made with these electrodes on a microsecond time scale and with micrometer spatial resolution. In addition measurements can be made and highly resistive solutions. A chronic electrode implant is an electronic device implanted chronically for a long period of time into the brain or other electrically excitable tissues. It may record electrical impulses in the brain or may stimulate neurons with electrical impulses from an external source. Microscopic electrodes can be implanted into the human anatomy at the speed of light by means of a electromagnetic radiation wave that of which is transmitted from an electrical device and would leave microscopic openings throughout the human body. The microscopic electrodes record and correlate to electrical impulses throughout the internal and external human anatomy of which the microscopic electrodes transforms the anatomical impulse data into a form of low frequency radio radiation. Therefore an Obama Electronic stalker can manipulate our biology into a giant sensor, that of which is linked to advance Computers and satellites. Microscopic electrodes are unable to function within the intricate in neural circuitry with precision. In contrast with tissue as a result their performance degrades over time, microscopic magnets (which are half a millimeter in diameter) that are electrically energized micro magnet positioned next to a neuron will then produce a chemical reaction through a magnetic field. A microscopic magnet can direct the stimulus of a neuron. Microscopic magnets are also capable of manipulating the nervous system and affecting the retina of the eye. Microscopic magnets can induce abnormally painful muscle tension of which can cause an immense amount of physical illness. Microscopic magnets are capable of affecting the digestive system by manipulating the cellular composition of the internal organs; in order to release poisonous chemicals that of which will cause internal illness. Nanorobots, Morgellons disease, and grey goo all possess artificial DNA and messenger RNA fragments; that of which is artificial genetic material that has been organized to pair up and bond together in order to form a microscopic computer. The artificial microscopic computers are capable of calculating and correlating data from digital sound waves produced by pulse modulated radio signals, wherein the microscopic computers built from artificial DNA and RNA fragments can through the instructions of the binary codes of the pulse modulated digital sound waves produce genetic light production that of which will dictate cellular activity by triggering chemical reactions and releasing poisons within the cells. The artificial DNA fragments of Nanobots, Morgellons disease, and grey goo share a common ability of bonding with other molecules. Artificial DNA fragments found in nanorobots, Morgellons disease, and grey goo can construct two-dimensional patterns, three dimensional objects, and simple shape changing devices. Complex programmable machines uses DNA molecules that of which follows a programmable path has been modified in combining multiple DNA devices to make an assembly line. The Nano contraption picks up gold nanoparticles as it tumbles along a DNA pattern surface. Digital sound waves and light radiation can program nanorobots to manipulate molecules found within cells by relocating the molecule and eradicating parts of the molecule in order to form or create chemical reactions that will cause a new molecule to exist. Artificial Gene synthesis is a method in synthetic biology that is used to create artificial genes in the laboratory. Currently based on solid phase DNA synthesis it difference from molecular cloning and polymerase chain reaction (PCR) in that the user does not have to begin with existing DNA sequences. Therefore it is possible to make completely synthetic double-stranded DNA molecules with no apparent limits on either nucleotide sequence of size. The method has been used to generate functional bacterial or yeast chromosomes containing approximately 1 million base pairs. Recent research also suggests the possibility of creating novel nucleotide base pairs in nature, which could greatly expand the possibility of expanding the genetic code, DNA printer builds genes from electronically submitted sequences and clones them directly into a vector. Optogenetics is a biological technique which involves the use of light to control cells in living tissue, typically neurons that have been genetically modified to express light-sensitive all your channels it is a neural modulation method employed in Neuroscience that uses a combination of techniques from Optogenetics to control and monitor the activities of individual neurons in living tissue, even within freely moving animals and to precisely measure the effects of the manipulations in real-time the key reagents used in optogenetics are light sensitive proteins. Neuronal control is achieved using Optogenetics activities such as Channelrhodopsins, halorhodopsin, and archaerhodopsin, wow Optical recording of neuronal activities can be made with the help of Octogenetics sensors for calcium, vascular release, neurotransmitters, or membrane voltage. The process of light emission from a DNA and our messenger RNA molecule requires the scientific understanding of the Quantum Leap which is as follows a photon is emitted because of an electron that falls and or drops from a higher state to a lower energetic state, this then releases a photon. This photon is used to get an electron into a higher state, so it can resonate again. Each atom responds to certain wavelengths, each atom would osculate due to the wavelength that is radiated, every atom is a resonator for certain specific wavelengths. Photons can make electrons jump from a lower to a higher state of energy state, this releases energy and or information. Atoms can store light and emit light depending on how long it is needed for each item to reach a certain state there is a light Network between all apps of a DNA double helix molecule and that of a messenger RNA molecule. Biophotons that are emitted from a DNA and or messenger RNA molecule causes hundreds of thousands of chemical reactions every second these reactions take about a nanosecond. All chemical reactions are controlled by the biophotons. Coherence is an orderly process to keep the biophotons from colliding together and so that there will be order. Energy can only be transferred in small units called quanta Planck's constant (h). The word quantum derives from quantity and refers to a small packet of action or process, the smallest unit of either that can be associated with a single event in the microscopic world. Changes of energy, such as the transition of an electron from one orbit to another around the nucleus of an atom, is done in discrete quanta. Quanta are not divisible. The term quantum leap refers to the abrupt movement from one discrete energy level to another, with no smooth transition. There is no ``inbetween''. Quantization limits the energy to be transferred to photons and resolves the UV catastrophe problem. The electron travels in a circular orbit around the nucleus. The orbit has quantized sizes and Energies. Energy is emitted from the atom, when the electron jumps from one orbit to another closer to the nucleus. Shown here is the first Balmer transition in which an electron jumps from orbit n = 3 to orbit n = 2, producing a photon of red light with an energy of 1.89 eV and a wavelength of 656 x 10 to the -9 m. The Bohr model basically assigned discrete orbits for the electron, multiples of Planck's constant, rather than allowing a continuum of energies as allowed by classical physics.The power in the Bohr model was its ability to predict the spectra of light emitted by atoms. In particular, its ability to explain the spectral lines of atoms as the absorption and emission of photons by the electrons in quantized orbits. Line Spectra are characteristics of the elements that emit the radiation line Spectra are also called atomic spectra, because the lines represent wavelength radiated from atoms when electrons change from one energy level to another. The molecular composition of a nanorobot, grey goo nanobot and smart dust are capable of affecting a person psychologically and physically. Molecular robots and or molecular machines are able to manipulate the mental emotional state of a person by triggering billions of chemical reactions within the neurons of the human brain. There are certain kinds of nanorobots, grey goo nanobots, and smart dust molecules that have been specifically designed for the limbic system structure of the brain and have been technologically categorized under four different groups of nanorobots, grey goo nanobots, and smart dust particles. The four different groups of nanorobots, grey goo nanobot, and smart dust particles that belong to the limbic system structure of the brain are as follows the thalamus nanobot, the thalamus grey goo the thalamus smart dust particle, the amydala nanobots, the amygdala grey goo, the amygdala smart dust particle, the hippocampus Nanobots, the hippocampus grey goo, the hippocampus smart dust particle, the hypothalamus nanobot, the hypothalamus grey goo, and the hypothalamus smart dust particle. The thalamus Nanobots, the thalamus grey goo, and the thalamus smart dust in abstract terms are molecular robots, molecular machines, and molecular computers that are implanted within the cells of the thalamus tissues of the limbic system found within the diencephalon. By means of digital sound waves propagated from any electronic device and or electronic equipment such as "microwave towers, radio towers, and satellites," the thalamus nanorobots, the thalamus grey goo nanobots, and the thalamus smart dust particles are provided binary instructions that will program the microscopic computers, that of which are DNA and RNA fragments found within the thalamus Nanobots, thalamus grey goo, and too are the smart dust particles. Biophotons are emitted throughout and in between the molecular structure of artificial DNA and RNA fragments and too are the biophotons transferred as a current to the natural molecular structure of the human DNA and RNA molecules, wherein more biophotons are emitted. This will result in a chain of chemical reactions that of which will change the cellular activities in the thalamus. The change of cellular activities within the thalamus will result in the artificial manipulation of the human senses of "sight, smell, hearing, taste, and touch" the thalamus grey goo nanorobots are capable of self-replicating themselves within the cells of the thalamus and are too capable of manipulating molecules within the cells of the thalamus in order to form more Thalamus Grey Goo Nanorobots; that will control the chemical composition of the thalamus as a result the emotional state of an individual will be artificial. The amygdala Nanorobots, the amygdala grey goo, and the amygdala smart dust particles are specifically designed to control the feelings of anger, violence, fear, and anxiety of which are formed by the chemical reactions that take place within the amygdala of the diencephalon. This process wherein the Amygdala nanorobots, amygdala grey goo, and amygdala smart dust particles manipulate our feelings of anger, violence, fear, and anxiety can only be achieved as long as a digital sound wave is provided to the molecular robots, molecular machines, and the molecular computers, that of which has been propagated from any electronic device and or electronic equipment. The amygdala nanorobots, amygdala grey too, and the amygdala smart dust particles are capable of destroying the amygdala my causing a set of chemical reactions based upon the amygdala nanobots, amygdala grey goo, and the amygdala smart dust particles light production as a result the amygdala Nano robots, amygdala grey goo, and amygdala smart dust particles cause a mailing effect of which forces the amygdala to undergo hyperorality, hypersexuality, and disabled behavior. The hippocampus Nanorobot, hippocampus grey goo, and the hippocampus smart dust particles have been uniquely designed by Nano scientists to mimic the genetic material of the hippocampus as a result of the biophotons light radiation production of the hippocampus Nanorobots, hippocampus grey goo, and hippocampus smart dust particles; new memories can be formed in the hippocampus. Digital sound waves transmitted by an Obama electronic stalker from any electronic device and or electrical equipment will be program the hippocampus nanorobots, hippocampus Grey Goo Nanobots, and the hippocampus smart dust particles to emitwhichhotons from the DNA and RNA fragments found within the hippocampus Nanorobots, hippocampus Grey Goo, and the hippocampus smart dust particles that of which will cause billions of chemical reactions in the cells of the hippocampus. The chemical reactions will result in the transfer of short-term memory to long-term memory. The hippocampus Grey Goo nanorobots are capable of self-replicating and are also capable of manipulating molecules that of which forms the anatomy of the hippocampus, intermoor hippocampus Grey Goo Nanobots. Therefore our short-term memories and long-term memories may one day be completely artificial and programmed, I am a victim of Obama's Grey Goo mind control. My memories are at all times programmed and artificial my memories appear to be computerized video sequences of events. The light emission of the hypothalamus Nanorobots, hypothalamus grey goo, and hypothalamus smart dust causes chemical reactions within the cells of the hypothalamus that of which will regulate the autonomic nervous system by controlling the endocrine system through the release of hormones into our bloodstream. The hypothalamus Nanobots, hypothalamus grey goo, and the hypothalamus smart dust are capable of controlling and regulating our hunger, thirst, sleep, and sex. Atomically Precise Manufacturing(APM) is the production of materials, structures, devices, and finished goods in a manner such that every atom is at its specified location relative to the other atoms, and in which there are no defects, missing atoms, extra atoms, or incorrect (impurity) atoms.
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A transmitter of a cell phone takes the voice of an individual that is using the cell phone and encodes it onto a continuous sine wave. A sine wave is a continuously varying wave that radiates out from the antenna and fluctuates evenly through space. Sine waves are measured in terms of frequency, which is the number of times a wave oscillates up and down per second. Once the encoded sound has been placed on the sine wave, the transmitter sends the signal to the antenna, which then propagates the electromagnetic radiation wave out of the cell phone.
Cell phones contain low power transmitters built inside of them. A cell phone operates on about 0.75 to 1 watt of power. The position of a transmitter inside a phone varies depending on the manufacturer, but it is usually in close proximity to the phone's antenna. The radio waves that send the encoded signal are made up of electromagnetic radiation propagated by the antenna. The function of an antenna in any radio transmitter is to launch the radio waves into space; in the case of cell phones, these waves are picked up by a receiver in the cellphone tower.
Electromagnetic radiation is made up of waves of electric and magnetic energy moving at the speed of light, according to the Federal Communications Commission (FCC). All electromagnetic energy falls somewhere on the electromagnetic spectrum, which ranges from extremely low frequency (ELF) radiation to X-rays and gamma rays. Given the fact that cell phones can transmit radio wave at an extremely far distance, the antenna of a cell phone is able to transmit radio and microwave signals into the human anatomy. Therefore microchips within cell phones have been designed to calculate a person’s position in the form of a sensor. Cell phone microchips possess integrated microscopic transistor circuits that transforms the cell phone into a pocket size portable sensor. An electronic stalker can hack the programs of the cell phone in order to radiate microwave radiation waves that of which can sense and or determine a person's location as the person moves through the propagated radiation waves. Cell phones can transmit radio radiation waves that can penetrate a person's skull and interact with a individual's brain. Given the fact that neurological nanobots and microscopic electrodes can transform the light of a person's DNA and can also compile and correlate the data of neurological electrical impulses into radio wave data, a cell phones radiation waves can pick up and measure a person's neurological radio wave data. A cell phone is capable of transmitting the neurological radio waves the receiving microwave tower, wherein the data is sent to a Obama electronic stalker and thus the user of the cell phone has had his or her thoughts read and recorded. A cell phone's electromagnetic radiation frequency ranges between (3 kHz to 3000GHz). Radio frequency (RF) electromagnetic radiation (EMR) is the transfer of energy by radio waves. RF EMR lies in the frequency range between 3 kilohertz (kHz) to 300 gigahertz (GHz). RF EMR is non-ionisingradiation, meaning that it has insufficient energy to break chemical bonds or remove electrons (ionization). Microwaves are a form of electromagnetic radiation with wavelengths ranging from one meter to one millimeter; with frequencies between 300 MHz(100 cm) and 300 GHz (0.1 cm). This broad definition includes both UHF and EHF (millimeter waves), and various sources use different boundaries. The human auditory response to pulses of radio frequency (RF) energy, commonly called RF hearing, is a well-established phenomenon. Effective radio frequencies range from 2.4 to 10000 MHz, but an individual's ability to hear RF induced sounds is dependent upon high frequency acoustic hearing in the kHz range above about 5 kHz. The site of conversion of RF energy to acoustic energy is within or peripheral to the cochlea, and once the cochlea is stimulated, the detection of RF induced sounds in humans and RF induced auditory responses in animals is similar to acoustic sound detection. The fundamental frequency of RF induced sounds is independent of the frequency of the radio waves but dependent upon head dimensions. The auditory response has been shown to be dependent upon the energy in a single pulse and not on average power density. The weight of evidence of the results of human, animal, and modeling studies supports the thermoelastic expansion theory as the explanation for the RF hearing phenomenon. RF induced sounds involve the perception via bone conduction of thermally generated sound transients, that is, audible sounds are produced by rapid thermal expansion resulting from a calculated temperature rise of only 5 x 10(-6) degrees C in tissue at the threshold level due to absorption of the energy in the RF pulse. The hearing of RF induced sounds at exposure levels many orders of magnitude greater than the hearing threshold is considered to be a biological effect without an accompanying health effect. This conclusion is supported by a comparison of pressure induced in the body by RF pulses to pressure associated with hazardous acoustic energy and clinical ultrasound procedures. Therefore it has been scientifically proven that cell phones can transmit pulse modulated radio radiation waves in the frequency range of (5 kHz to 10000MHz). Given the fact that our government is investing billions of US tax paying dollars into the advancements of cell phone technology, there is a high possibility that all modern cell phones such as "smart phones and androids," are more than capable in modulating, calculating, correlating, and transmitting radiation waves within the RF hearing spectrum. Cell phone microchips contain microscopic integrated transistor circuits that are designed to give Obama electronic stalkers the ability to transmit radio signals similar to a remote control that transmits radio signals at a directed destination. Therefore an Obama electronic stalker can measure and detect a person's location through satellites and microwave radiation that is released by the cell phone and once the individual's location is tracked, an Obama electronic stalker can then transmit a pulse modulated radio signal within perfect accuracy to a person's skull. Our cell phones can also propagate light radiation from the screens of our cell phones and possibly other parts of a cell phone that of which causes a unique form of digital effects on a person's vision. Our cell phones are weapons of mind control mass destruction! The technology found within a cell phone is also found within all electronic devices, therefore all electronic devices can track a person, sense the location of a person, direct electromagnetic signals at a person's specific body part such as the brain, and ultimately brain wash and monitor the thoughts of a person. There are radiation waves that can distort and eradicate the pulse modulated radio and microwave radiation waves and other forms of mind control radiation waves similar to QuWave technology. Our government under Obama is extremely unwilling to propagate the neutralizing radiation waves from microwave towers that would protect people from the rapid abundance of pulse modulated radiation waves that is found all around the country of which controls our thoughts. Sound waves are the patterns of vibrations of disturbance caused by the movement of energy traveling through a medium of any solid, liquid, or gaseous matter. As the sound waves propagate away from the origin of the sound. The source of the vibration is the location wherein the sound waves first originate, that of which would be classified as a type of object. The sound vibration manipulates the particles in the surrounding medium through a disturbance; a chain of particle disturbances emerge. The pattern of particle disturbances creates an outward movement in the form of a wave pattern. The wave carries the sound energy through the medium, usually in all directions and less intensely as it moves farther from the source. There are two forms of "audio recordings," which are analog and digital. Methods that replicate the audio recording are considered analog. Digital is recorded by taking samples of the original sound wave at a specific rate. Digital audio is technology that can be used to record, store, generate, manipulate, and reproduce sound using audio signals that have been encoded in digital form. Obama Electronic stalkers use a method of programming people by prerecording entire specific demands in the form of artificial thoughts that of which are transmitted from a common electronic device to a victim of electronic harassment through low frequency pulse modulated analog radio signals. However if the Obama stalker aims at manipulating a persons thoughts by means of programming illegal implanted "nanobots, grey goo, black goo, Morgellons disease, smart dust, and or microscopic electrodes," a digital sound wave is most often used to genetically manipulate the Obama victim. Digital sound waves are used to program the artificial DNA fragments of a molecular robot and or molecular machine. Binary data encoded within an electric signal sent and or transmitted by an Obama electronic stalker, are capable of reprogramming our electronic devices, of which are electronic weapons in disguised. Under Obama's dictatorship within the United States; if a person desires to write, talk, think, blog, and or protest the crimes of electronic harassment through Nanobot mind control torture, Obama's electronic stalkers will attack the individual by manipulating the person's thoughts and forcing physical restraint on to the person without an outside physical force. As a result of the attacks of mind control against the victims of electronic harassment; the individuals will be forced to forget crucial details of their pursuit against electronic harassment. The same is done too many other victims of electronic harassment worldwide within fascist grey goo countries such as "China and Russia." All life forms on planet "Earth" and nature itself are now being programmed. Nanorobots is the technology of creating molecular machines and or molecular robots at a microscopic scale of one billionth of a meter, "a nanometer." The use of CMOS (CMOS a technology for making low power integrated circuits,) with the respective advances of nanowires are used to enable embedded sensors for manufacturing nanorobots. Nanobots are applied to hydrology monitoring systems. Nanorobots are useful for agriculture or environmental monitoring and management. The Innovative approach to evaluate hydraulic conductivity, considering nanorobotics as a new paradigm to enable more precise analysis in the field of hydrology monitoring. The applications of nanorobotic for agricultural purposes and monitoring water and soil qualities may result in a impressive impact towards environmental control; in terms of increasing and decreasing the pollution among many different natural species. A total market for nanotechnology-based environmental applications in the year of 2005 was evaluated as 374.9 million dollars and by the year 2010 this market reached more than 6.1 billion dollars. The advantages and disadvantages of using nanorobots for environmental applications are as follows, more control in terms of measuring microorganisms, creating microorganisms, expanding the amount of microorganisms, better detection of pollution, creating solutions, and improved control of water temperature. Grey Goo is both a nanotechnology substance which increases exponentially without practical limits and a hypothetical scenario in which the mass of the planet Earth or the universe itself has been consumed into self-replicating Nanobot. A molecular assembler is a kind of molecular machine, some biological molecules such as ribosomes fit this definition; this is because they received instructions from messenger RNA and then assemble specific sequences of amino acids to construct protein molecules. Robotic molecular Manufacturing Systems or assemblers, these nanoscale robots can perform many different tasks; such as roaming the bloodstream, dissolving blood clots, and killing cancerous cells. However, in order for this process to occur, wherein "Grey Goo Nanobots" perform medical applications; there must firstly be an abundance of Grey Goo Nanobots injected and/or implanted within an individual's anatomy. Although there is a theoretical possibility wherein, one Grey Goo Nanobot can self replicate and also manipulate molecular substances, so that more artificial Grey Goo Nanobots can then emerge. The major threat is that grey goo Nanobots will expand onto all matter and thus will change the molecular composition of the matter into more Nanobots, of which will transform all carbon matter into grey goo. In order for this grey goo scenario to occur, the molecular machines must be able to survive in a variety of harsh environments. The grey goo Nanobots would also need the technological capabilities to consume any and all organic matter. The grey goo nanorobotic assemblers is created to convert organic matter into other materials, the assembler is programmed to create new units identical to itself, each new unit follows the same programming instructions to consume and multiply, the molecular manufacturing rate becomes exponential; producing an increasing amount of assemblers constantly. Eventually the assemblers would strip the Earth of all organic matter, thus leaving only nanomachines behind. Black goo functions very similarly to our genetics however black goo does not need DNA it is sufficient to have a special type of mineral oil coated with gold and iridium M state condition basically we have the same M State pattern sprayed within the DNA of any living being on the planet most planets might have this Collective conscious black goo substance there are two types of black goo one made by the earth and the other landed here by attention through a meteor swarm 80000 years ago. The black goo substance in simple terms is a seed device, the intelligence that seeded the off world goo has created and is creating life by passing the natural order and bringing life forms to a higher level of order than they should naturally be. The out of world alien black goo requires energy in order for it to spread and survive the frequencies that the alien black goo is running on as an energy source can utilize emotional fields with a very low vibration, which means it needs to create pain and fear to feed on. The technology that this AI introduced to this planet has learned to utilize the birth of biophotons coming out of beings when they suffer and when they die. There are two parts of biophotons; there is the visible pattern that we can observe or kill and the invisible part which is about 97% of all biophotons within all humans. The moment an organism dies, the light production of that specific organism's DNA molecule has then lost coherence and thus a sudden burst of biophotons, that of which is like an energetic shock wave that can be redirected, and used for purposes. There are two functions of stealing energy one is to feed the internal intelligence long-range the other one is to achieve certain goals. Black goo is an alien and or Earthly substance that can be synthetically created from the earth and or alien based black goo substances, that of which will then be classified as a form of nanotechnology. Morgellons disease a form of nanotechnology that is self-replicating hollow Fischer, that of which transforms the light production of an organism's DNA into radio signals the radio signals that Morgellons disease creates is propagated out of an organism's body and is detectable by satellite and ground station Morgellons disease is a computer virus that can cause horrible skin disorders characterized by sores crawling Sensations on and Under the Skin and fiber-like filaments emerging from The Source it is thought that the fiber like filaments are a result of an infectious process process in the skin cells Morgellons disease symptoms are as follows, skin sores that causes dramatic physical deformity where in an individual may lose one or all of the five senses and or may lose a particular body part such as the limbs and or face, insect-like crawling sensations on and under the skin in the form of moving stinging or biting, severe bleeding out of the source of the skin, the possibility of one's eye color changing to red, fiber threads or black stinging materials in and on the skin, severe fatigue, difficulties in concentration, short term memory loss dizziness, and depression. The synthetic molecular structure of Morgellons disease is identical to the molecular composition all bacteria, viruses, fungi, single and multicellular parasites, and includes suggestions of normally non-pathogenic organisms as well as Environmental contamination. Morgellons disease is a skin disease which seems to be similar to a multi system disease. Morgellons disease appears to be a parasite like infection. Most registered Morgellons disease patients are known to live in the United States. The number of Morgellons disease patients is steadily increasing in Europe as well. Chemtrails are chemical and biological agents of Morgellons disease which are deliberately sprayed and left in the sky by flying aircrafts contrails that dissipate relatively quickly are considered to be normal however contrails that do not dissipate must contain additional substances. The purpose of the release of the Morgellons disease Chemtrails are as follows, solar radiation management, psychological manipulation, human pollution Control, weather modification, or biological or chemical warfare. The trails are causing respiratory illness and other health problems. Chemtrails are formed at high altitudes (5 to 10 miles or 8 to 16 kilometres long.) The Grey goo Dictator "Barack Hussein Obama" is indirectly responsible for the increasing number of Morgellons disease Chemtrails in the United States, the fascist grey too fascist dictators "Barack Hussein Obama, Michelle Obama, Joe Biden, and Hillary Clinton" have ordered their Grey Goo agents to propagate Morgellons disease molecules from light sources that provide marijuana plants energy. The Morgellons disease molecules that are propagated from the light sources belong to the molecular structure of "bacteria, viruses, fungi, single and multicellular parasites." This process of propagating Morgellons disease can occur in one's own household. Morgellons disease molecules can be transmitted from any electronic device within a person's household and or community. Smart dust a collective of microelectromechanical systems forming a simple computer in a container light enough to remain suspended in air, used mainly for information-gathering in environments that are hostile to life. Smart dust is a system of mainly tiny microelectromechanical systems (MEMS)such as sensors robots or other devices that can detect for example light, temperature, vibration, or chemicals. They are usually operated on a computer network wirelessly and are distributed over sensing through radio frequency identification. Without an antenna of much greater size. The range of a tiny smart dust Communications device is measured in a few millimeters and they may be vulnerable to electromagnetic disablement and destruction by microwave exposure. Smart dust particles can monitor everything, acting like electronic nerves endings for the planet. Fitted with computing power sensing equipment, wireless radios, and long battery life. Smart dust particles are capable of making observation of real-time data about people, cities, and the natural environment. Intelligent dust particles embedded in the brain could form an entirely new form of brain machine interface. The real time monitoring of brain function has advanced in leaps in recent years. That's largely thanks to various new technologies that can monitor the collective behavior of groups of neurons, such as functional magnetic resonance Imaging, magneto encephalopathy and position emission tomography. Each particle of neural dust consists of standard CMOS circuits and sensors that measure the electrical activity of neurons nearby. This is coupled to a piezoelectric material that converts ultra high frequency sound waves into electrical signals and vice versa. The neural dust is interrogated buy another component Place beneath the scale but powered from outside the body. This generate the ultrasound that powers the neural dust and sensors that listens out for their responses, gather like an RFID system. The system is also featherless the data is collected and stored outside the body for later analysis. The system is lower-power, can have a high spatial resolution, and it is easily portable. It is also rug and can potentially provide a link over long periods of time a major hurdle in brain-machine interfaces (BMI) is the lack of an implantable neural interface system that remains visible for a lifetime. Smart dust particles that are on a scale of roughly 100 micrometers to that of a nanometer are capable of sending or receiving signals in the harsh, warm, and noisy environment. Within the body, smart dust particles use ultrasound to send and receive data. At this scale, smart dust would generate a damaging amount of heat because of the amount of energy the body absorbs and the traveling signals to noise ratio at this scale. Ultrasound is a much more efficient and should allow the transmission of at least ten million times more power than electromagnetic radiation waves at the same scale a major danger of smart dust is the cost of monitoring of people by implanting the particles within the environment smart dust particles are capable of traveling within and electromagnetic radiation waves the electromagnetic waves are transmitted from a common electrical device such as a "television, radio, stereo, security alarm, digital camera, light bulbs, computer desktops, laptops, and much more." Smart dust particles that are transmitted through electromagnetic radiation wave, exist outside of an organism. Therefore this would indicate a difference of power usage and power absorption within the smart dust particles; thus allowing the smart dust to exist within all electromagnetic radiation Spectrums. Therefore it is possible that smart dust can obtain digital radio wave data. Microscopic electrodes can be used to make measurements that are difficult or impossible with conventional electrochemical techniques. Measurements of chemical concentration can be made with these electrodes on a microsecond time scale and with micrometer spatial resolution. In addition measurements can be made and highly resistive solutions. A chronic electrode implant is an electronic device implanted chronically for a long period of time into the brain or other electrically excitable tissues. It may record electrical impulses in the brain or may stimulate neurons with electrical impulses from an external source. Microscopic electrodes can be implanted into the human anatomy at the speed of light by means of a electromagnetic radiation wave that of which is transmitted from an electrical device and would leave microscopic openings throughout the human body. The microscopic electrodes record and correlate to electrical impulses throughout the internal and external human anatomy of which the microscopic electrodes transforms the anatomical impulse data into a form of low frequency radio radiation. Therefore an Obama Electronic stalker can manipulate our biology into a giant sensor, that of which is linked to advance Computers and satellites. Microscopic electrodes are unable to function within the intricate in neural circuitry with precision. In contrast with tissue as a result their performance degrades over time, microscopic magnets (which are half a millimeter in diameter) that are electrically energized micro magnet positioned next to a neuron will then produce a chemical reaction through a magnetic field. A microscopic magnet can direct the stimulus of a neuron. Microscopic magnets are also capable of manipulating the nervous system and affecting the retina of the eye. Microscopic magnets can induce abnormally painful muscle tension of which can cause an immense amount of physical illness. Microscopic magnets are capable of affecting the digestive system by manipulating the cellular composition of the internal organs; in order to release poisonous chemicals that of which will cause internal illness. Nanorobots, Morgellons disease, and grey goo all possess artificial DNA and messenger RNA fragments; that of which is artificial genetic material that has been organized to pair up and bond together in order to form a microscopic computer. The artificial microscopic computers are capable of calculating and correlating data from digital sound waves produced by pulse modulated radio signals, wherein the microscopic computers built from artificial DNA and RNA fragments can through the instructions of the binary codes of the pulse modulated digital sound waves produce genetic light production that of which will dictate cellular activity by triggering chemical reactions and releasing poisons within the cells. The artificial DNA fragments of Nanobots, Morgellons disease, and grey goo share a common ability of bonding with other molecules. Artificial DNA fragments found in nanorobots, Morgellons disease, and grey goo can construct two-dimensional patterns, three dimensional objects, and simple shape changing devices. Complex programmable machines uses DNA molecules that of which follows a programmable path has been modified in combining multiple DNA devices to make an assembly line. The Nano contraption picks up gold nanoparticles as it tumbles along a DNA pattern surface. Digital sound waves and light radiation can program nanorobots to manipulate molecules found within cells by relocating the molecule and eradicating parts of the molecule in order to form or create chemical reactions that will cause a new molecule to exist. Artificial Gene synthesis is a method in synthetic biology that is used to create artificial genes in the laboratory. Currently based on solid phase DNA synthesis it difference from molecular cloning and polymerase chain reaction (PCR) in that the user does not have to begin with existing DNA sequences. Therefore it is possible to make completely synthetic double-stranded DNA molecules with no apparent limits on either nucleotide sequence of size. The method has been used to generate functional bacterial or yeast chromosomes containing approximately 1 million base pairs. Recent research also suggests the possibility of creating novel nucleotide base pairs in nature, which could greatly expand the possibility of expanding the genetic code, DNA printer builds genes from electronically submitted sequences and clones them directly into a vector. Optogenetics is a biological technique which involves the use of light to control cells in living tissue, typically neurons that have been genetically modified to express light-sensitive all your channels it is a neural modulation method employed in Neuroscience that uses a combination of techniques from Optogenetics to control and monitor the activities of individual neurons in living tissue, even within freely moving animals and to precisely measure the effects of the manipulations in real-time the key reagents used in optogenetics are light sensitive proteins. Neuronal control is achieved using Optogenetics activities such as Channelrhodopsins, halorhodopsin, and archaerhodopsin, wow Optical recording of neuronal activities can be made with the help of Octogenetics sensors for calcium, vascular release, neurotransmitters, or membrane voltage. The process of light emission from a DNA and our messenger RNA molecule requires the scientific understanding of the Quantum Leap which is as follows a photon is emitted because of an electron that falls and or drops from a higher state to a lower energetic state, this then releases a photon. This photon is used to get an electron into a higher state, so it can resonate again. Each atom responds to certain wavelengths, each atom would osculate due to the wavelength that is radiated, every atom is a resonator for certain specific wavelengths. Photons can make electrons jump from a lower to a higher state of energy state, this releases energy and or information. Atoms can store light and emit light depending on how long it is needed for each item to reach a certain state there is a light Network between all apps of a DNA double helix molecule and that of a messenger RNA molecule. Biophotons that are emitted from a DNA and or messenger RNA molecule causes hundreds of thousands of chemical reactions every second these reactions take about a nanosecond. All chemical reactions are controlled by the biophotons. Coherence is an orderly process to keep the biophotons from colliding together and so that there will be order. Energy can only be transferred in small units called quanta Planck's constant (h). The word quantum derives from quantity and refers to a small packet of action or process, the smallest unit of either that can be associated with a single event in the microscopic world. Changes of energy, such as the transition of an electron from one orbit to another around the nucleus of an atom, is done in discrete quanta. Quanta are not divisible. The term quantum leap refers to the abrupt movement from one discrete energy level to another, with no smooth transition. There is no ``inbetween''. Quantization limits the energy to be transferred to photons and resolves the UV catastrophe problem. The electron travels in a circular orbit around the nucleus. The orbit has quantized sizes and Energies. Energy is emitted from the atom, when the electron jumps from one orbit to another closer to the nucleus. Shown here is the first Balmer transition in which an electron jumps from orbit n = 3 to orbit n = 2, producing a photon of red light with an energy of 1.89 eV and a wavelength of 656 x 10 to the -9 m. The Bohr model basically assigned discrete orbits for the electron, multiples of Planck's constant, rather than allowing a continuum of energies as allowed by classical physics.The power in the Bohr model was its ability to predict the spectra of light emitted by atoms. In particular, its ability to explain the spectral lines of atoms as the absorption and emission of photons by the electrons in quantized orbits. Line Spectra are characteristics of the elements that emit the radiation line Spectra are also called atomic spectra, because the lines represent wavelength radiated from atoms when electrons change from one energy level to another. The molecular composition of a nanorobot, grey goo nanobot and smart dust are capable of affecting a person psychologically and physically. Molecular robots and or molecular machines are able to manipulate the mental emotional state of a person by triggering billions of chemical reactions within the neurons of the human brain. There are certain kinds of nanorobots, grey goo nanobots, and smart dust molecules that have been specifically designed for the limbic system structure of the brain and have been technologically categorized under four different groups of nanorobots, grey goo nanobots, and smart dust particles. The four different groups of nanorobots, grey goo nanobot, and smart dust particles that belong to the limbic system structure of the brain are as follows the thalamus nanobot, the thalamus grey goo the thalamus smart dust particle, the amydala nanobots, the amygdala grey goo, the amygdala smart dust particle, the hippocampus Nanobots, the hippocampus grey goo, the hippocampus smart dust particle, the hypothalamus nanobot, the hypothalamus grey goo, and the hypothalamus smart dust particle. The thalamus Nanobots, the thalamus grey goo, and the thalamus smart dust in abstract terms are molecular robots, molecular machines, and molecular computers that are implanted within the cells of the thalamus tissues of the limbic system found within the diencephalon. By means of digital sound waves propagated from any electronic device and or electronic equipment such as "microwave towers, radio towers, and satellites," the thalamus nanorobots, the thalamus grey goo nanobots, and the thalamus smart dust particles are provided binary instructions that will program the microscopic computers, that of which are DNA and RNA fragments found within the thalamus Nanobots, thalamus grey goo, and too are the smart dust particles. Biophotons are emitted throughout and in between the molecular structure of artificial DNA and RNA fragments and too are the biophotons transferred as a current to the natural molecular structure of the human DNA and RNA molecules, wherein more biophotons are emitted. This will result in a chain of chemical reactions that of which will change the cellular activities in the thalamus. The change of cellular activities within the thalamus will result in the artificial manipulation of the human senses of "sight, smell, hearing, taste, and touch" the thalamus grey goo nanorobots are capable of self-replicating themselves within the cells of the thalamus and are too capable of manipulating molecules within the cells of the thalamus in order to form more Thalamus Grey Goo Nanorobots; that will control the chemical composition of the thalamus as a result the emotional state of an individual will be artificial. The amygdala Nanorobots, the amygdala grey goo, and the amygdala smart dust particles are specifically designed to control the feelings of anger, violence, fear, and anxiety of which are formed by the chemical reactions that take place within the amygdala of the diencephalon. This process wherein the Amygdala nanorobots, amygdala grey goo, and amygdala smart dust particles manipulate our feelings of anger, violence, fear, and anxiety can only be achieved as long as a digital sound wave is provided to the molecular robots, molecular machines, and the molecular computers, that of which has been propagated from any electronic device and or electronic equipment. The amygdala nanorobots, amygdala grey too, and the amygdala smart dust particles are capable of destroying the amygdala my causing a set of chemical reactions based upon the amygdala nanobots, amygdala grey goo, and the amygdala smart dust particles light production as a result the amygdala Nano robots, amygdala grey goo, and amygdala smart dust particles cause a mailing effect of which forces the amygdala to undergo hyperorality, hypersexuality, and disabled behavior. The hippocampus Nanorobot, hippocampus grey goo, and the hippocampus smart dust particles have been uniquely designed by Nano scientists to mimic the genetic material of the hippocampus as a result of the biophotons light radiation production of the hippocampus Nanorobots, hippocampus grey goo, and hippocampus smart dust particles; new memories can be formed in the hippocampus. Digital sound waves transmitted by an Obama electronic stalker from any electronic device and or electrical equipment will be program the hippocampus nanorobots, hippocampus Grey Goo Nanobots, and the hippocampus smart dust particles to emitwhichhotons from the DNA and RNA fragments found within the hippocampus Nanorobots, hippocampus Grey Goo, and the hippocampus smart dust particles that of which will cause billions of chemical reactions in the cells of the hippocampus. The chemical reactions will result in the transfer of short-term memory to long-term memory. The hippocampus Grey Goo nanorobots are capable of self-replicating and are also capable of manipulating molecules that of which forms the anatomy of the hippocampus, intermoor hippocampus Grey Goo Nanobots. Therefore our short-term memories and long-term memories may one day be completely artificial and programmed, I am a victim of Obama's Grey Goo mind control. My memories are at all times programmed and artificial my memories appear to be computerized video sequences of events. The light emission of the hypothalamus Nanorobots, hypothalamus grey goo, and hypothalamus smart dust causes chemical reactions within the cells of the hypothalamus that of which will regulate the autonomic nervous system by controlling the endocrine system through the release of hormones into our bloodstream. The hypothalamus Nanobots, hypothalamus grey goo, and the hypothalamus smart dust are capable of controlling and regulating our hunger, thirst, sleep, and sex. Atomically Precise Manufacturing(APM) is the production of materials, structures, devices, and finished goods in a manner such that every atom is at its specified location relative to the other atoms, and in which there are no defects, missing atoms, extra atoms, or incorrect (impurity) atoms.
2016.11.01 19:26 GingerpithicusFrisii 40M w/ ADD needs a good analogy through which to learn genetics. And maybe a tutor.
X-post ADHD
This is sort of hard to explain, so please bear with me. I'm 40 years old, and I want to go to grad school in a genetics-related field. From what I know of genetics, I really like it, but due to some bad experiences in the past, I have a sort of mental "wound" when it comes to getting a grasp on some of the concepts. Because of my ADD, when I'm confronted by a problem that I can't immediately grasp, I feel really stupid, and the shame associated with that feeling creates a sort of mental "block" that confuses the situation so badly that I have an extremely difficult time engaging with the material. Having said that, I'm looking for an analogy through which to engage with the material. The best one I can think of at this point is that of cooking/baking/recipe, i.e. a recipe is the instructions for an organism. How can I expand this analogy to explain things like alleles, genetic drift, and homozygosity, among others? Something that seems to help me is accurate visual representations of the processes and the various "things" that do the work, i.e. watching a CGI animation of a ribosome.
submitted by GingerpithicusFrisii to IWantToLearn [link] [comments]
This is sort of hard to explain, so please bear with me. I'm 40 years old, and I want to go to grad school in a genetics-related field. From what I know of genetics, I really like it, but due to some bad experiences in the past, I have a sort of mental "wound" when it comes to getting a grasp on some of the concepts. Because of my ADD, when I'm confronted by a problem that I can't immediately grasp, I feel really stupid, and the shame associated with that feeling creates a sort of mental "block" that confuses the situation so badly that I have an extremely difficult time engaging with the material. Having said that, I'm looking for an analogy through which to engage with the material. The best one I can think of at this point is that of cooking/baking/recipe, i.e. a recipe is the instructions for an organism. How can I expand this analogy to explain things like alleles, genetic drift, and homozygosity, among others? Something that seems to help me is accurate visual representations of the processes and the various "things" that do the work, i.e. watching a CGI animation of a ribosome.
2016.06.14 00:41 NotEdgarAllenPoe [High School Honors Biology] A couple questions on DNA and RNA
My teacher just wants me to answer these questions. I looked all throughout the provided reading, and had quite a bit of trouble finding the answers
submitted by NotEdgarAllenPoe to HomeworkHelp [link] [comments]
- If mRNA codons are AUG, GGU, CAG, what three codons of tRNA will attach?
- In an analogy between a factory and a cell: If DNA is the superintendent and mRNA is the order to the assembly line (ribosomes) what might be the role of tRNA?
- If the DNA analysis of a gene shows 20% adenine bases, what would be the percentage of thymine, guanine, and uracil?
- What might be the result of a mutation of DNA in which a triplet code such as CAC now says CTC?
2015.03.27 19:39 p_h_scale School Project- I have to come up with an analogy for a plant or animal cell that includes the different organelles and their functions
So basically, I was just dropped a project for which I have no ideas. The project is to create a poster on the cell of a plant or animal, but depicting the cell using a clever analogy. (For example, if the cell was a mall, the information desk would be the nucleus) There are certain organelles that have to be covered, such as:
Nucleus, Nucleolus, Cell Membrane, Protien, Endoplastic Reticulum, Golgi Apparatus, Ribosome, Mitochondria, and Lysosome.
Could someone help me? I kind of understand the organelles but it's hard for me to think of a suitable analogy for the cell. Some other students in mas class are choosing to do a theme park. Anyone have any cool ideas on an alanolgy i could use?
Thanks in advance
submitted by p_h_scale to biology [link] [comments]
Nucleus, Nucleolus, Cell Membrane, Protien, Endoplastic Reticulum, Golgi Apparatus, Ribosome, Mitochondria, and Lysosome.
Could someone help me? I kind of understand the organelles but it's hard for me to think of a suitable analogy for the cell. Some other students in mas class are choosing to do a theme park. Anyone have any cool ideas on an alanolgy i could use?
Thanks in advance