"According to mainstream scientists and chronologists, based on uranium-lead series radiometric dating of moon rocks the Earth is only 4.6 billion years old therefore years did not exist before that because the Earth wasn't orbiting the Sun." [emphasis added]
I really wish I had a witty retort here, but I'm dumbstruck at the sheer ignorance.
Oh, Nephilimfree, you've done it again. You went and dragged genetics through the mud again, and I won't stand for it.
At this point, having dedicated a few posts to his inane ramblings, debunking Nephy's claims is beginning to feel like picking on the fat kid at the playground. He's a slow, lumbering target, and all the other kids on the playground keep picking on him because he's easy prey. But Nephy is so ripe with nonsense, so overflowing with vacuous crap like a bountiful cornucopia of bullshit, that it's hard to resist tearing his arguments apart when I'm looking for something to write about. And his silly website [Edit: 06/11/11: Looks like Nephy has let his registration of his domain lapse, so that link doesn't work any more. I tried to find an archived version, but had no luck] has no shortage of fodder for a creationist asskicking.
This week, I took a look at this article he wrote about the enzyme nylonase. You've probably heard about nylonase before, as it is often given as a great example of an evolutionary adaptation that has occurred in recent history. In 1975, a team of researchers from Osaka University in Japan got the idea to try and culture sludge obtained from the waste water outside of nylon factories1. The samples they collected were used as inocula, and added to cultures which contained a form of nylon (6-aminohexanoic acid cyclic dimer) as the sole carbon and nitrogen source. Any bacteria that grew would have to rely on metabolizing nylon to survive. And grow they did. They designated the strain as KI72, and after isolating the bacteria, they identified it as a strain of Achromobacter guttatus, although later work by the same team reclassified the species as a strain of Flavobacterium2. A few years later, the researchers identified two novel enzymes which allow the bacterium to metabolize nylon: 6-aminohexanoic acid cyclic dimer hydrolase and 6-aminohexanoixc linear oligomer hydrolase (6-AHA CDH and 6-AHA LOH, respectively)3,4. Since nylon production began in the 1930s, these enzymes had to have originated in the time since then. After all, it doesn't make much sense for a bacterium to have produced enzymes to specifically degrade nylon before nylon itself was invented. These genes, then, represent an example of a novel adaptation arising outside of the lab and within the past century.
But Nephy disagrees. He states,
"Because the bacteria encountered nylon and developed an ability to digest it does not provide evidence of any kind of evolutionary change. This ability does not effect the form and structure (morphology) of the bacteria by introducing any new structural feature, nor does it transform any existing structural feature of the bacteria into a new kind of structure with a new physiological function."
Two paragraphs in, and he's already run into a major problem. He seems to have this odd idea that unless a change results in gross morphological alterations, it cannot be an evolutionary change. He simply discredits novel biochemical adaptation out of hand without any sort of justification. He simply wishes to define evolution as changes in "form and structure" and ONLY changes in "form and structure" - any other kind of change he refuses to acknowledge as evolutionary change. In essence, he's defining evolution in his own incredibly narrow terms, so that any actual evolutionary change can be shrugged off as "not evolution". If we were to narrowly define creationism as "the spontaneous formation of aardvarks from forest detritus", it would be pretty easy to discredit, too.
But beyond that, it is simply silly to only accept large changes in morphology as the only kind of evolutionary change. Morphological alterations cannot occur all at once. Any modification to an organism's body plan would require many not-so-obvious biochemical changes to occur first - the very type of changes that Nephy does not accept as "evolution". Evolution can only work with what it has available. No organism is going to mutate and grow wings de novo all in one shot, even if it would be advantageous. Such changes would require modifying the existing body plan, and this would require extensive biochemical changes to happen first.
Nevertheless, the discovery of novel nylon-degrading enzymes is indisputable. Musing over the origins of these enzymes, Nephy declares that these proteins, or any protein, could not have simply evolved. No, he says, statistical analysis says otherwise:
"The field of sicence [sic] called Statistical Ananlysis [sic] which is employed to determine probability in various fields of science, has determined that the formation of proteins by random molecular interactions is on the order of 10^950, which is 1 to a number for which no name exists; a number greater than all of the paticles [sic] of matter in the speculated universe. In other words, according to science itself, the chance of a single, medium-sized protien [sic] arising by purely materialistic molecular interactions is considered impossible to science because it is considered impossible times impossible times impossible. The evolutionist would have you believe that random mutation is capable of producing novel protiens [sic] which have specific function, but this is not only unfounded but exceedingly irrational."
This is a typical creationist talking point: whipping out statistics to churn out large numbers and proclaim "See! It's statistically impossible for evolution to occur!" It is also typical, as Nephy demonstrates quite well, for creationists not to cite the source of these statistical calculations. The problem with Nephy's argument is that he does not take into account the process of selection during evolution. Forming a protein "randomly" and all at once is incredibly unlikely (though not entirely impossible), but if you factor selection into the equation, it becomes an incredibly likely phenomenon. Richard Dawkins illustrates this beautifully in his book The Blind Watchmaker, where he likens evolution to monkeys banging away at typewriters. If you were to wait for a monkey to type out the sentence "Methinks it is like a weasel", you'd be waiting for eons for it to "randomly" happen. But suppose you were to use cumulative selection to pick and keep the letters that work. Dawkins wrote a computer program to do just this (as computer programs are much cheaper and easier to work with than hordes of monkeys). Starting with a string of gibberish and then changing one letter per generation, the computer program "evolved" the correct sentence is about 40 generations5. It took only a few minutes for the computer program to complete this task, whereas single-step selection (waiting for the correct sentence to happen randomly, and all at once) would have taken the computer "a million million million million million years"6. Obviously, selection gets past the staggering statistical improbability that creationists argue.
But Nephy continues. He tells us that it was discovered that the nylonase genes originated from a frameshift mutation, resulting in an alternate reading frame which produced a novel enzyme7. This may be true, but recent work by Negoro et al indicates that the origin of the genes might be due to base substitutions after an ancestral gene duplication8. Nephy proceeds to tell us that there are only two ways that such a frameshift can occur: a random mutation or by a "Programmed Translational Frameshift Mutation".
At last, we come to the crux of Nehpy's argument. According to him, random frameshift mutations are invariably bad and the idea of a random frameshift mutation is a cop-out employed by "evolutionists" to ignore the reality of intelligent design. The origin of nylonase must be due to "Programmed Translational Frameshift Mutation", a process, he claims, is divinely inspired..
At this point I feel I should clear something up. Nephy, I hope you're reading. There is no such thing as "Programmed Translational Frameshift Mutation". Programmed Translational Frameshift (PTF) is a very real process, but it is not a mutation. PTF actually describes a variety of complex, but similar, processes. The essence of the idea is this: under normal circumstances, a protein is produced when a ribosome translates a strand of mRNA. Usually, the ribosome translates in a linear fashion, starting at the 5' end of the strand and reading the length of the strand until it comes to a stop codon at the 3' end. But in certain cases, the ribosome can be induced to "skip" or "hop" over a number of nucleotides in the sequence. The result is that the ribosome is shifted out of frame, and the resulting gene product is unlike the original9. With PTF, one gene sequence can produce multiple gene products: the original, unshifted, product and the second, shifted, gene product. This process is not a mutation. Mutations are changes to the genetic sequence itself, and such changes do not occur during PTF.
Perhaps Nephy's mistake stems from him being unable to comprehend the scientific literature. In his article, he describes PTF as "the modification of the arrangement of amino acids in a chain caused by information in the DNA which programs the event to occur", which is inaccurate, to say the least. This is further evidenced by the fact that he chooses to illustrate PTF with a diagram of alternative splicing, which is an entirely different process altogether! These errors would indicate that he simply did not understand what PTF is. I get the feeling that Nephy just skims through paper abstracts, pulling out words to form misshapen ideas, rather than taking the time to actually read any scientific papers.
But, regardless of whether or not PTF counts as mutation, Nephy's argument that nylonase originated due to PTF, rather than a simple frameshift mutation, doesn't hold much water. What we know about nylonase - the gene's sequence, how it is regulated, etc - would indicate that PTF is NOT at play here. As mentioned above, PTF occurs when a single transcript is read in two different reading frames, resulting in two different gene products. But in the case of nylonase, there is only ONE reading frame. It is always read by the ribosome in the same fashion. At no point is the ribosome prompted to switch to a new reading frame during translation - a hallmark of PTF. In many cases, this switch is induced by particular sequence elements, but the nylonase gene does not contain any such sequence elements. All evidence points to an ancestral gene that underwent a frameshift mutation that permanently altered it's reading frame, rather than two different and active reading frames from a single sequence. The original frameshift alteration was likely transcriptional in nature rather than translational.
Nephy's claim that random frameshift mutations are always harmful is nonsense as well. In any case where a mutation is deleterious, creationists are quick to say "See! Random mutations are bad!"; any case where a mutation proves to be beneficial, they shout "That didn't count! That was Intelligent Design!". This amounts to little more than special pleading. Nephy does not see it this way. He states
"The problem for evolutionists is that we have discovered that random frameshift mutations produce novel proteins which do not have a function in the cell, and when produced in great numbers, are causes of diseases such as Alzheimers and Tay-Sachs."
But how are deleterious mutations and non-functional proteins a problem for evolution? On the contrary, they are a huge problem for Creationists! After all, why would God allow for non-functional proteins to cause deadly conditions? Why would God allow for mutations to begin with? Pretty sloppy work for a Creator who is supposedly "perfect".
Another issue with his argument is how he ascribes PTF as an "intelligent design process". What evidence does he have that PTF is not a naturally occurring process? Why does he call it intelligent design? He gives no reason. He simply slaps the ID label on and announces "Hah! PTF proves intelligent design!" with no justification whatsoever. One could just as easily label espresso brewing "intelligent design" and proclaim that Starbucks baristas are evidence of divine creation. It is nonsensical.
So what it all comes down to is this: the nylonase gene is a product of a frameshift mutation and not programmed translational frameshift; programmed translational frameshift is not a mutation, nor is it evidence of Intelligent Design; biochemical adaptations do count as evolution; and nylonase still illustrates a wonderful example of evolution occurring within recent memory. Once again, Nephilimfree abuses genetics to form a murky mire of distorted truth, and once again, his claims do not stand up to the scrutiny of critical thought.
---------------------------------------------------------------------------------- 1. Kinoshita, S.; Kageyama, S., Iba, K., Yamada, Y. and Okada, H. (1975). "Utilization of a cyclic dimer and linear oligomers of e-aminocaproic acid by Achromobacter guttatus". Agricultural & Biological Chemistry39(6): 1219−23
2. Negoro, S.; Shinagawa, H.; Nakata, A.; Kinoshita, s.; Hatozaki, T. and Okada, H. (1980). "Plasmid control of 6-aminohexanoic acid cyclic dimer degradation enzymes of Flavobacterium sp. KI72". Journal of Bacteriology43(1): 238-245
3. Kinoshita, S.; Negoro, S.; Murayama, M.; Bisaria, V. S.; Sawada, S. amd Okada, H. (1977). "6-aminohexanoic acid cyclic dimer hydrolase . A new cyclic amide hydrolase produced by Achronobacter guttatus KI72" European Journal of Biochemistry. 80: 489-495.
4. Kinoshita, S.; Terada, T.; Taniguchi, T.; Takene, Y.; Masuda, S.; Matsunaga, N. and Okada, H. (1981). "Purification and characterization of 6-aminohexanoic-acid-oligimer hydrolase of Flavobacterium sp. KI72". European Journal of Biochemistry. 116(3): 547-551
5. Dawkins, R. (1986). The Blind Watchmaker, p. 48
6. Ibid. p. 49
7. Ohno, S. (1984). "Birth of a unique enzyme from an alternate reading frame of the preexisted, internally repititious coding sequence". Proceedings of the National Academy of Sciences. 81: 2421-2425
8. Negoro, S.; Ohki, T.; Shibata, N.; Sasa, K.; Hayashi, H.; Nakano, H.; Yasuhira, K.; Kato, D; Takeo, M. and Higuchi, Y. (2007). "Nylon-oligomer degrading enzyme/substrate complex: catalytic mechanism of 6-aminohexanoate-dimer hydrolase". Journal of Molecular Biology. 370: 142-156
This isn't going to be a long, lengthy post, but rather a short note on an interesting paper just published in Frontiers in Systems Neuroscience, detailing a neat advancement in ultramicroscopy.
As you probably already know, Drosophila is perhaps the most commonly used model organism in genetics. When a geneticist used Drosophila for a genetic screen, he generates mutants and then scans the progeny for particular desired phenotypes. For instance, if you're interested in a gene involved in the development of limbs, you'd generate mutants and then look for ones that have mutated legs. External phenotypes like this are pretty easy to observe, even without a microscope, but it's a bit harder when it comes to internal structures. What if your gene of interest is involved in forming the gut, or a particular set of muscles? One way you could go about observing internal structures would be to dissect your flies, but this has its limitations – it requires good manual dexterity, and has the added risk of tearing, ripping or otherwise mutilating your specimen. You could use in situ staining or florescence microscopy, but what you end up with is a flat 2-dimensional image that might not reveal all the details that would be present in three dimensions. Using a confocal microscope will give you good resolution, but generally use high magnifications that will not allow you to view your whole specimen at once. The paper by Jährling et al details a technique using ultramicroscopy that allows for an entire 3D reconstruction of a specimen, complete will internal structures visualized in situ.
The basic procedure goes like this: they began by "chemically clearing" their specimens – that is, using a series of chemical washes and incubations, they removed almost all colour from their specimens. They were left with flies which were nearly transparent. This would allow the internal structures to be visualized. The specimens were then mounted on an ultramicroscope, and using a laser, they took a series of 597 images, beginning at the top and moving down through the vertical plane. Once the images had been taken, they used specialized software to layer the images on top of one another to reconstruct a 3-dimensonal model. Since the flies were transparent, the model allowed for the visualization of internal structures as well as the specimen's surface. Using this technique, you can easily visualize internal structures that might be of interest to you without ever having to dissect your specimen or rely on 2-dimensional imaging techniques.
This technique really becomes powerful when coupled with fluorescent microscopy. Imagine you're convinced that your gene of interest plays a role in the development of the fly's gut. Attach GFP to a gut-specific promoter, insert the construct into your flies and then image them. What you'd get is a perfect 3D model of the fly's gut, easily distinguishable from surrounding tissue. Any phenotypic effects would be easy to observe! Using this technique, you could easily, quickly (the authors state that it takes about 30 minutes from start to finish) and reliably visualize any internal structure you wish. Pretty cool, no?
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References:
Jährling N, Becker K, Schönbauer C, Schnorrer F and Dodt H-U (2010). Three-dimensional reconstruction and segmentation of intact Drosophila by ultramicroscopy. Front. Syst. Neurosci. 4:1. doi: 10.3389/neuro.06.001.2010
It would seem that debunking Youtube creationists has become a hobby of mine. This week, I present a fellow by the name of MyGhettoGospel (I guess Jesus was into gangsta rap), who, for the sake of brevity, I'll refer to as MGG henceforth. MGG believes that biology can prove that the Bible is true, and presents his argument in the video below.
His argument is as follows: the Bible tells us that God "holds everything together"1. If it were not for God, he claims, everything would simply fall apart and the universe would be devoid of any sort of structure - and this includes people. Luckily for us, MGG says, biology provides evidence that this is indeed the case. The cells in our bodies are held together by adhesion molecules. One class of these molecules are laminins (or 'laminin's' as MGG seems to prefer). And, Great Scott, these molecules look like crosses. MGG has a picture and everything! What else could this be but the indelible mark of the Creator? A sound theological argument. Too bad it isnt reality.
MGG's argument falls apart for a variety of reasons. The first, and probably the biggest flaw in his argument is that laminin doesn't actually look like a cross. In his video, MGG states "If you look up laminins in any scientific medical piece of literature, this [the cross shape] is what you will see'. Well, I called MGG's bluff on this one and took a brief perusal through the literature. Here is an image taken from Denzer et al (1998)2:
Look much like a cross to you? Maybe, if it were constructed by a carpenter in a drunken stupor. How about this image from Beck, Hunter and Engel (1990)3:
Nope, still not a cross. I guess the literature does not support MGG's argument as strongly as he thinks. His error is in mistaking diagrams of laminin, like the one he presents, for the molecule's actual physical appearance. Diagrams of any molecular structure are stylistic representations. They are always drawn in a way that makes it easy to understand the basic structure of a molecule - where the domains are in relation to one another, how many peptide chains comprise the molecule and how they are linked together, for instance. They are not meant to be taken as representing precisely what the molecule looks like. There is always some creative liberty taken when designing a diagram. Laminin does not have a rigid cruciform structure. It resembles a cross only vaguely.
This vague cross-like shape shouldn't be in any way surprising to start with. A cross shape is very simple; it's just two lines running perpendicular to one another. Given the number of different types of proteins in the body and the variety of conformations that they can take on, it would be incredible if there weren't any proteins that resembled crosses. It can easily occur naturally and randomly. Imagine tossing toothpicks across a table. Given enough toothpicks, you're bound to find some that fall to form a cross. Would anyone argue that God had a role in this? I guess Divine Toothpicks aren't marketable.
But even if laminin did take on a rigid shape, who is to say that it depicts a cross? It could look like many things. Rotate it 90° and it looks like a dagger. I think you'd be hard pressed to find anyone who would claim this is a molecular representation of a Sikh's kirpan, and therefore Sikhism is the one true religion. The cross argument is equally absurd.
Another reason why MGG's argument is bunk is that it takes for granted the shape of Jesus' execution device as a cross. The shape of the cross has been branded into the public conscience for centuries but there is little historical reason for this. Implements for crucifixion took a variety of shapes. Writing 75 CE, the Roman historian Josephus commented that crucifixion was done in a variety of ways4. Indeed, crucifixion was sometimes done using wooden devices shaped like a T, like a Y or even like an X, as well as using the familiar cross shape. Is there any reason to believe that Jesus was crucified on a cross? Surprisingly, no. The word used in the Bible to describe Jesus' execution implement, in the original Greek, was "σταυρός" (stauros). This is translated as "upright stake" or "wooden post", indicating that he was nailed to a simple, single upright beam (known as a crux simplex). Plutarch and Lucian describe the stauros as having the form of the Greek letter Tau, or T. Neither of these interpretations can be taken as meaning a cross. So if Jesus being crucified on a cross is of dubious nature, so too is the laminin argument. If Jesus actually died on a simple wooden pole, then a cruciform molecule has no significance.
MGG's argument is also problematic theologically. The structure of laminin predates the supposed crucifixion of Christ by many millions of years. Even by Creationist standards, the crucifixion did not occur until thousands of years after Creation. Why would God decide to use a design based on the cross, then? Did he have foreknowledge that Jesus was to be crucified? This would indicate that Jesus was destined to die on the cross for mans' sins. And if Jesus was destined to die on the cross, then mankind was destined to sin. This sort of deterministic implication is at odds with the rest of theology, which claims that God gave man free will and that sin is a choice. MGG's argument implicates the opposite. Which is it, MGG? You can't have it both ways.
In essence, MGG's argument fails. Not only does laminin not resemble a cross, but even if it did, it wouldn't make any sense to interpret it as as sign from a Creator. Creationists, please stop polluting molecular biology with your nonsense. Besides, we all know who really holds us all together.
1. "The Son is the image of the invisible God, the firstborn over all creation. For in him all things were created: things in heaven and on earth, visible and invisible, whether thrones or powers or rulers or authorities; all things have been created through him and for him. He is before all things, and in him all things hold together" Collosians 1:15-17
2. Alain J. Denzer et al. Electron microscopic structure of agrin and mapping of its binding site in laminin-1 . The EMBO Journal (1998) 17, 335–343, doi:10.1093/emboj/17.2.335
3. Konrad Beck, Irene Hunter, and Jürgen Engel . Structure and function of laminin: anatomy of a multidomain glycoprotein . The FASEB Journal . 4(2), 2148-2160
I love DNA. It is a wonderfully complex molecule and the mechanisms whereby genetic information is stored and accessed is fascinating; and yet, at the same time, the basic premise by which is works - the "central dogma" of molecular biology - is beautifully simple. There is little wonder why DNA has caught the eye of the public in a way that few other biological compounds have. This fascination with DNA has necessitated trying to explain the concepts underlying genetics to the public. Therein lies a problem for scientists and science journalists: how to convey the intricate and often confusing workings of science in a way that is both interesting and easy to understand for the layperson. The one tool brandished about the most is the metaphor. Unfortunately, the metaphor can be dangerous, and there is no better example of this than those metaphors used to explain DNA. Two unfortunate metaphors for DNA have been devised: the idea that DNA functions as a "blueprint" and the idea that DNA functions like a "computer code".
The 'blueprint' metaphor is especially poor. Consider what a blueprint is, exactly. It is a scale schematic used to represent a structure. If you have a blueprint of a hotel, you have a schematic of how to build that hotel. The blueprint tells you everything you need to know - how high the ceilings are, how long each wall is, how many steps are in each flight of stairs. Furthermore, you know that 1 inch on the blueprint represents, say, 1 meter in the actual hotel. From the blueprints, you can precisely construct the hotel. But there is more to a blueprint than this. The information conveyed in a blueprint works both ways - you can use a blueprint to construct a hotel, and from a fully constructed hotel, you can derive a blueprint. If a wall in the hotel is 3m in length, you can draw a wall on the blueprint 3 inches long. The information is reversible. You can go from blueprint to structure and from structure to blueprint.
This is where the analogy with DNA fails. DNA does not work as a blueprint because the information is not reversible. DNA does contain information necessary to construct an organism, but if you examine a fully formed organism, you cannot reconstruct the original DNA sequence. You cannot measure the length of a nose or determine the colour of an eye, and then write out the specific sequence needed to create these features. This is a very important aspect of a blueprint, and DNA does not meet this requirement. Rather, DNA acts more like a recipe. A recipe tells you what ingredients you need and in what manner to combine them in order to create a pie. But if you have a pie, you cannot examine it, even in the most minute of detail, and work out the exact recipe that was used. The information contained in a recipe is not reversible, just as the information spelled out by our genes is not reversible.
The 'computer code' metaphor is also a poor one, for multiple reasons (this particular analogy was popularized by Discovery Institute lackey Stephen C. Meyer). The way a computer code works is that the exact sequence of the code - the precise order of the binary 1s and 0s - spells out exactly what operations the computer must perform. But in genetics, the sequence is only part of the picture. Just as important are genetic regulatory networks - which genes are turned on at what times and in combination with which other genes. Phenotypes are not simply the result of particular gene sequences but the result of specific gene-gene (or gene network-gene network) interactions.
But DNA bears little relation to a "code" in a more fundamental way. Consider exactly what a "code" is. A code is a system of arbitrary symbols used to represent ideas and objects. In a sense, language itself is a "code"; the symbol "dog" represents that furry tetrapod with a waggly tail, for example. In a code, the symbols themselves have no inherent meaning. The letter "d" is meaningless by itself, as are the letters "o" and "g". It is only in combination that they derive meaning, and their meaning is derived from the idea that they represent. Furthermore, they only have meaning because we give them meaning. "Dog" is merely the label we apply to Fido; in a universe without sentient beings, "dog" would be meaningless. DNA does not fit this description at all. DNA is not arbitrary in any way; each letter of the genetic "code" is an actual biological compound. ACCGTCGA might be the gene for determining how long your toe hair is, but unlike a code, A, C, T and G each have their own non-arbitrary meaning. And this meaning exists independently of human sentience - the sequence of nucleotides does not have meaning only because we give it meaning. It would have meaning even if humans didn't exist at all.
What DNA is, is a polymeric chemical that follows a dynamic chemical process, governed by universal physical rules. It is only a "code" in the same sense that nuclear fusion is a "code" for how stars produce light
So why am I taking the time to mention these things? The reason is because both these weak metaphors have been abused time and time again by creationists (and particularly the Intellignent Design IDiots). Just recently, the video below was posted to Youtube by Nephilimfree, who you may recall from my last blog post (to which he made no attempt to refute, despite having been made aware of my critique - something that should probably come as no surprise to anyone, given the tendency for creationists to retreat with tail planted firmly between their legs when presented with cold, hard, scientific fact). This latest video does not appear to be made by Nephy himself (though he gives no credit to the video's creator), but is nonetheless filled to the brim with that Nephy-brand distortion of science. While it is significantly shorter than his last few 14-minute diatribes, it might still result in significant impairment to your mental faculties, so watch at your own risk.
The video wastes no time in misleading the viewer, tossing out the "blueprint" metaphor 39 seconds in: "DNA contains the blueprint of all life and is by far the densest information storage mechanism known in the universe". For reasons stated above, we know this metaphor is misleading at best and deceptive at worst. But it continues: "The program code and design of such an incredible system indicated a supremely intelligent designer".
Now, a claim like that one is pretty bold, and would require pretty strong evidence to rationally accept it as fact. So what kind of evidence does the video provide? The answer, really, is "none". It immediately cuts to clips of creationist talking heads (Ken Ham, Dave Hunt, and the like) who reiterate one point: "DNA is a code, and codes are information, which only comes from intelligence". Yet, at no point do they present one shred of evidence for why this is the case. They expect the viewer to simply take what they say as being true. Here we have a major distinction between science and creationism - any scientific claim will be backed up by evidence and cite sources explaining why the claim is true, whereas creationism makes assertions which they simply expect you to believe.
The video proceeds to give some details of DNA - it is self-replicating, has error-correction mechanisms ("there are special proteins called enzymes...making repairs" announces Frank Sherwin - a statement that could only be more generic had he said "there are chemicals that do stuff"), etc. But throughout, a unifying theme is repeated - "these things are complex and only God can produce complexity". But again, they provide no reason why we should believe this is true. Perhaps it is left up to our imagination.
What the video boils down to is that creationists make two claims about DNA: 1) that DNA is a "code", and 2) information/complexity (via the genetic code) can only come from an intelligent designer. Both these claims are really nonsense.
Calling DNA a "code", as explained above, is simply incorrect. DNA is not a code in any sense of the word. But let's assume for a moment, that DNA is a code written by God. If this were the case, then God could definitely benefit from taking an introductory computer programming course. God seems to be an awful coder. DNA is very error prone, and the code is regularly mistranslated and copied incorrectly. Different organisms have similar functions, but use different coding sequences. Some organisms contain the code for functions they don't even use, and the majority of code in any given organism is completely non-coding! For an all powerful supreme being, his code is awfully amateurish.
The argument that "information and complexity can only come from intelligence" is also absurd. To begin with, whenever creationists fling around the term "information" they never define what it is they mean by the term. "Information" can mean different things in different contexts. To a creationist, information is some amorphous concept, never, or only vaguely, defined. The idea that "information" cannot be arranged by nature is also silly. Consider the following situation. A friend says to you, "The sun has to have been created by an intelligent creator. There is no other way to explain sunlight." "Don't be silly," you retort. "The sun is a burning ball of hydrogen which emits energy with wavelengths in the visible spectrum." Unfazed, your friend replies, "That is nonsense. Consider the sources of light we have here on Earth. We only ever see light from light bulbs. Light bulbs do not arise naturally! They are the produce of man made design. We never see light occurring naturally. The sun has to have been intelligently designed. Chemicals cannot just come together and "randomly" create light!". Such an argument is not unlike that creationists use to explain genetic information. They claim that genetic information has to have been designed because information does not arise spontaneously; but the claim that information does not arise spontaneously assumes that genetic information was designed! Once again, a creationist argument is little more than tautology.
In the end, the argument presented in Nephy's little video can basically be paraphrased as "Look at DNA! Look at it! Isn't it complex?! And look at cells! They are soooooo complex!", and then baselessly ascribing that complexity to God. This is, of course, patently untrue. There are many examples of complexity arising through completely naturalistic mechanisms. Snowflakes are a perfect example of this. Do creationists really think that their God spends time making each individual snowflake? What about crystals? Pour some sugar into hot water and suspend a string in it, and before long, you have beautiful and complex crystalline growth. This is an entirely natural process - complexity without the intelligence.
Complexity is not the hallmark of design. DNA is not a blueprint nor is it a computer code. And once again, Nephilimfree is not correct.
Nephilimfree, Youtube creationist extraordinaire and posterboy for the giant headphone lobby, has posted a new video entitled "Overlapping and Embedded Genes". Unfortunately for him, I am a lover of any and all things genetic. Also unfortunately for him, he doesn't have a clue what he's talking about. Fortunately for me, this provides me an opportunity to tear his video to shreds.
A little background may be necessary. Nephilimfree (who I will henceforth refer to as "Nephy", as I am an avid believer of making infuriatingly inane things tolerable by giving them cute names) made this video in response to a conversation he had with Sofiarune. He does not mention it, but I was also involved, as I am Sofiarune's go-to guy for molecular biology. I guess you can say I have a personal interest in this video, but I'd pick apart Nephy's claims in any event since they are, as usual, stupid on a Goats On Fire level.
First, the video. Be warned, it is rather long, running at just over 14 minutes. If you don't have the time (or the patience) to watch the whole thing, I'll give you the tl;dr (...or is that tl;dw...) version below. Go grab some coffee, because this post is gonna be a long one.
Nephy's argument is basically this: (i) the existence of overlapping genes is an obstacle to evolution because a single mutation will be deleterious to multiple genes and (ii) these gene pairs could not have possibly evolved and are thus evidence that they have been created. As we will see below, both of these points are patently false, and they demonstrate the extent to which Nephy is ignorant of both evolution and genetics.
Nephy starts the video off by mentioning his discussion with Sofiarune, and his insistence that genes overlap and that this is somehow proof that evolution isn't true. He states that "being the evolutionist that she is, she said 'No, no, no. Genes are read linear and they are not embedded'." Nephy is only telling a half truth here. In their original conversation, he presented "overlapping genes" in a very different manner than he does in this video, as the figure below demonstrates:
So Nephy broached the subject with a cryptic sentence about overlapping sequences "causing entropy" to "the code". Understandably, Sofia asked for clarification. In response, he talked about overlapping sequences in shotgun sequencing. This is entirely different. Overlapping sequences in shotgun sequencing and overlapping genes in the genome are not the same thing - one is a bioinformatic technique used to align sequence data in the proper order and the other is the idea that sequences can have multiple open reading frames (ORFs) coding for different gene products. He followed this up with a link to an article [not shown] which further obfuscated what he had meant. It talked about how, in the early days of molecular biology, there was debate over how the genetic code was read; were sequences read in one long linear manner, or were all three possible reading frames of a sequence read at once, resulting in overlapping sequences? It was determined early on that the correct answer was the former - codons were read one at a time in a linear fashion. In this context, Sofia was entirely justified in saying that genes did not overlap. Nephy seemed to have gotten all these concepts confused, but in his video, he presents it as if he gave Sofia a concrete definition of "overlapping genes". Leave it to a creationist to be vague, only to misrepresent your response.
Nevertheless, Nephy now has a concrete definition: overlapping genes are multiple coding ORFs contained within a sequence. Such overlapping genes do exist, primarily in RNA viruses. A study done by Chirico et al1 (which I will go into some detail below) found that 75% of the 2000 or so known species of virus have some extent of gene overlap. This does not mean that it is a widespread phenomenon as Nephy seems to believe. He points to an article entitled Mammalian Overlapping Genes: The Comparative Perspective2 and is seemingly impressed by the numbers. It shows a total of 774 total overlapping genes in the human genome, and this might be impressive to Nephy, but it isn't to anyone who actually took the time to read the paper. This 774 is out of the 34,604 annotated gene sequences posted to the NCBI human genome assembly (build 33). That's a whopping 2.2% of genes. So overlapping genes in humans are more the exception than they are the rule. This is the same for pretty much all eukaryotic organisms; overlapping gene sequences do exist, but they are pretty rare. They are mostly seen in viruses (indeed, overlapping sequences were first discovered in he late 1970s by researchers working with the phage φX174). Nephy talks about overlapping genes as if they are as numerous as the grains of sand on the beach, but they are actually quite infrequent.
But Nephy isn't only concerned with the existence of overlapping genes. He claims that overlapping genes are a problem to evolutionists. He thinks this is because a mutation in the overlapping sequence would be deleterious to both genes and evolution could never favour such a situation. This is demonstrably false, and the evolution of overlapping genetic sequences can, and has, been explained. A paper by Rancurel et al.3 (2009) did just that. According to the authors, there are two characteristics of overlapping genes that alleviate evolutionary constraints on them: (i) overlapping proteins are full of amino acids with a high level of codon degeneracy and (ii) the regions of proteins encoded by overlapping sequences have a tendency towards structural disorder. It is worth going into some detail about these.
(i) To understand what the first point means, you will need to understand what is meant by "codon degeneracy". There are 64 different codons which can be constructed from the four nucleotides, but only 20 main amino acids which comprise any polypeptide. This means that there will be some amino acids that are encoded by multiple codons. Arginine, for example, has 6 different codons - CGU, CGC, CGA, CGG, AGA, and AGG. You'll notice that these codons are pretty similar to each other, and that is pretty handy for the cell. If, for instance, a mutation changes a CGU codon into CGC, CGG or CGA, it will still encode for arginine. The sequence has changed, but the output of the sequence remains the same. The mutation will have no effect on the protein sequence. This is what is meant by codon degeneracy. Amino acids with codon degeneracy will be able to tolerate some degree of mutation. This is important to overlapping genes, because the proteins produced by overlapping genes are high in amino acids that have codon degeneracy. What this means is that mutations to the sequence can be tolerated and won't have a deleterious effect. This is quite the opposite of what Nephy claims. He feels that a mutation will be doubly deleterious to overlapping genes, and he would be right if it weren't for the high frequency of codon degeneracy found in these proteins. In many cases, a mutation will have no effect at all on either protein in the pair.
ii) Structural disorder describes the extent to which the 3D structure of a protein is defined. Those proteins with a high degree of order have a strictly defined 3D secondary structure, while those with a high degree of structural disorder do not. They tend to rapidly change from one structural form to another - their secondary structure is not strictly defined. Since it is the amino acid sequence of a polypeptide that largely determines it's 3D shape and thus function, those with a high degree of structural disorder can tolerate some degree of mutation. Mutations will not affect the protein's 3D shape much because it doesn't have a definite shape to begin with. As the authors put it, "[d]isordered proteins are generally subject to less structural constraint than ordered ones". It should not be surprising, then, that the regions of proteins which are encoded by overlapping sequences tend to be structurally disordered. Those parts do not have a rigid secondary structure, so mutations will have less of a deleterious effect on these overlapping regions. Again, this is antithetical to Nephy's claim that mutations in overlapping genes are a death sentence for a cell.
As an aside, this point about structural disorder raises an interesting theological question: if overlapping genes were created by God as Nephy believes, then why did God decide to create proteins which have regions of structural disorder? If he created these proteins for a particular reason, then would he not have designed them all to have a definite 3D structure that belies their function? Did God just get lazy and figure "Eh, I'll just make some of these proteins structurally ambiguous. No one's gonna notice"? From a design perspective, it doesn't make sense, especially when the designer is perfect and all powerful. Why would he even design overlapping genes to begin with? Wouldn't he just stick to the good old "one gene = one gene product" plan? It's much simpler. It's a hallmark of poor design when things are more complicated than they need to be. How can a perfect God have an imperfect design, anyway?
So Rancurel and co. have thoroughly shown Nephy's point on mutation to be bunk. But they also give his claim that overlapping genes could not have evolved a thrashing. In fact, they do this in the very first paragraph of their paper! They state:
"Among several mechanisms, they [overlapping gene pairs] can be created by a process called "overprinting", in which a DNA sequence originally coding only one protein undergoes a genetic modification leading to the expression of a second reading frame in addition to the first one...The resulting overlap encodes and ancestral "overprinted" protein region and a protein region created de novo (i.e., not by duplication) called an "overprinting" or "novel" region" [See figure below, click to embiggen].
In other words, overlapping gene pairs can be explained easily by a natural process. Two genes exist with reading frames shifted relative to one another, with one upstream from the other. The loss of a stop codon in the upstream gene results in this gene being extended into the region of the second gene where it ends at a stop codon. The result, then, is two genes which share a region of sequence. This has an important evolutionary consequence. The novel region is free to take on novel cellular functions. For the reasons stated above, the novel region is under fewer constraints. In fact, the creation of proteins de novo in this manner has likely played a very important part in viral evolution4. In many viruses, the novel protein in overlapping protein pairs are virulence factors or encode enzymes that allow the virus to escape host defence mechanisms. De novo creation of novel proteins by overlapping genes represents another mechanism by which novel "information" is added to the genome, something creationists love to deny is possible.
But not only can we explain how overlapping proteins pairs have evolved but we also have some good ideas why they would evolve. Chirico et al give four possible reasons why overlapping gene sequences may have evolved in viruses.
Mutation rates: given the high mutation rates seen in viruses, it makes sense that there is pressure on viruses to keep their genomes short. Longer genomes will accrue more mutations than shorter ones. Overlapping genes are a way for a virus to expand its repertoire of genes without extending its genome.
Capsid size: some viruses have capsids of limited size. Increasing the size of these capsids to accommodate increased genome sizes is quite the undertaking and is likely to have a fitness cost. Thus it would be advantageous for the virus to have genes which overlap, since this takes up less space within the capsid.
Gene length: larger genomes tend to have less overlap than smaller genomes. This might be because there is more room in larger genomes for the genes. Viruses may have overlapping genes simply because they have small genomes and cannot fit all the genes linearly.
Expression regulation: it is possible that overlapping genes evolved so that the genes in a gene pair can be regulated together.
The authors studied the sequence data from 62 different virus families to see which of the four possibilities best matched. They determined the likely cause for the evolution of overlapping genes in viruses was the constraint caused by capsid size. Nonetheless, it is entirely possible that any of the other three may have occurred in certain cases.
The reason I bring this up is because science has at least made an attempt to explain why overlapping genes exist at all. Nephy and his creationist brethren are content to claim that God created overlapping genes but they don't say a word about why he would have done so. The naturalistic explanation offered by evolution not only explains how but also why. The explanatory power of evolution is massive, while creationism offers little more than just-so stories and ad hoc justifications.
But despite all this, Nephy talks for 9 minutes about how overlapping genes are evolutionarily impossible, while saying absurd things like "Geneticists today are shying away from the use of the word 'gene' because it really doesn't describe what we observe in the genome of life. The preferred term is 'sequences' because it is difficult to say what code ends where and starts where in some cases". As someone with a degree in molecular genetics, this took me by surprise. No one sent me that memo! This statement makes little sense; genes and sequences are not equivalent, and it's actually pretty easy to determine where one sequence starts and one sequence ends. We've even been able to develop computer software that can predict such things in a matter of milliseconds. Given that Nephy has little scientific background and is definitely not part of the geneticist community, I'd like to know just where he got the idea that the term "gene" was passé. It's still very much a useful term and is used constantly in the scientific literature.
He finishes off his video with a five minute snippet of a talk given by Hubert Yockey. I find it amusing that Nephy introduces this clip by saying "And now a few select moments from a lecture by a geneticist", followed immediately by a screen declaring "Biophysicist Hubert Yockey". Nephy, a biophysicist and a geneticist are not the same thing. Not even close. And Yockey isn't even a biophysicist to begin with; he's a physicist. He did some work on information theory and how it applies to biology, but this does not make him a biophysicist. I know these are big words for you, but do try to understand the distinction between them before you toss them around again. I won't actually go through the claims made by Yockey in the video (to be honest, I didn't even watch that part) because really, a physicist's claims about biology are about as meaningful as a butcher's claims about nuclear physics.
So once again, Nephilimfree has demonstrated that he has no idea what he is talking about. Overlapping gene sequences are NOT evidence of Divine creation - they make no sense if one assumes they were created, and they make perfect sense when interpreted in the light of evolution. We have a perfectly naturalistic explanation of their origin which conforms to experimental observation. Furthermore, mutations within overlapping genes are not always a bad thing, and have likely contributed to the evolution of pathogenicity in many species of virus. His claim that mutations in overlapping genes are always deleterious is patently nonsense. In fact, at one point in the video he claims that "all genetic mutations cause degretory[sic] effects to the genome's code", a claim that literally thousands of examples can disprove. He says that he has told evolutionists this for a long time and they "refuse to listen". There's a simple reason for that, Nephy - it's because you're flat out wrong.
Consider this a challenge, Nephy. Show me how what I have written is incorrect. Show me why the authors I have quoted are wrong - critique their work. Give me evidence taken from peer-reviewed scientific literature that backs up your claims, and not just idle speculation on your part. Give me a thorough refutation, thoroughly sourced. Because until you do your claims will be little more than verbal diarrhea.
1. Nicola Chirico, Alberto Vianelli and Robert Belshaw. Why genes overlap in viruses. Proceedings of The Royal Society Biological Sciences . 2010 . 277: 3809-3817
2. Vamsi Veeramachaneni et al. Mammalian overlapping genes: the comperative perspective . Genome Research . 2004 . 14:280-286
3. Corinne Rancurel et al. Overlapping genes produce proteins with unusual sequence properties and offer insight into de novo protein creation . Journal of Virology . 2009 . 83(20): 10719-10736
4. F. Li and S. W. Ding . Virus counterdefence: diverse strageties for evading the RNA-silencing immunity. 2006 . Annual Review of Microbiology . 60:503-531
Going over my blog stats today I noticed something odd. I wrote a post two years ago about the interesting discovery of a virus that uses another virus as it's host. This actually seems to be the most popular thing I've written on my blog - it has about twice as many views as the next most viewed piece. In the last two days it has had quite a few views, and this is not odd, but I did notice that someone had found it by googling "cwgk.blogspot.com/2008/08". Kinda weird. I was curious what kind of search results that would turn up, so I tried it myself, and I found only four results: three were from my blog (expected) and one more from a forum called RevivalSermons.org.
Ok, so some Bible lover linked to my virus post on a religious forum. That in itself is kinda strange. But not as strange as what I found when I clicked on the link...
"Virus > could viruses and prions be Satan's attempts to create the building blocks of life - unsucessfully [sic] - or just a Satanic weapon ?"
This was followed by four links to different sites that talked about the virus dead/alive debate, mine being the first. I have no idea how my blog post supports the poster's idea that viruses are some kind of satanic weapon. To be honest, I'm kinda creeped out.
"A U.S.-led research team may have finally located the lost city of Atlantis, the legendary metropolis believed swamped by a tsunami thousands of years ago in mud flats in southern Spain."
The team of scholars used underground mapping, and deep-ground radar to uncover structures buried beneath swampy mud flats north of the city of Cadiz. But, why are they so certain that they've found the fabled Atlantis?
"Freund's discovery in central Spain of a strange series of "memorial cities," built in Atlantis' image by its refugees after the city's likely destruction by a tsunami, gave researchers added proof and confidence, he said.
Atlantis residents who did not perish in the tsunami fled inland and built new cities there, he added."
So their evidence that they have found Atlantis is that they found "memorial sites" to the North that they attribute to being built by Atlantean refugees. But what makes them so sure these "memorial sites" are Atlantean in origin? Well, because they're north of the possible site of Atlantis, of course! If you don't see a problem with this, then you should probably take a refresher course in circular arguments.
But there's more reason to be skeptical. Which journal is the team planning on detailing their findings? Well, none.
"The team's findings will be unveiled on Sunday in "Finding Atlantis," a new National Geographic Channel special."
Because revealing your findings in a made-for-TV documentary is something legitimate scholars do, right? Though this should come as little surprise; the team is being lead by "Dr." Richard Freund - a guy who's PhD is from the Jewish Theological Seminary, has also claimed to have found the lost treasures of the Temple of Jerusalem, and has written a book called “Secrets of the Cave of Letters: A Dead Sea Mystery”. The guy is little more than a "reality-show" historian and comparable to the likes of Zecharia Sitchin and Eric Von Daniken. In other words, the guy's a crank.
Also, why is it that any time a submerged structure is discovered, people cry "AH-HA! Atlantis!"? The evidence that Atlantis even existed is dubious at best, and even if it did, a sunken city is probably hardly unique. "Atlantis" has already been found dozens of times. While Freund's find is interesting itself, it is not "Atlantis".
Not much in the way of science in this post, just something I had been musing about for a while.
Among people of the religious persuasion, there seem to be three main camps of people when it comes to attitudes towards evolution. There are those who outright deny evolution is possible - the Ken Hams and Ray Comforts of the world - and a large chunk of time is often dedicated to debunking the asinine claims of these nutjobs. There are those creationists who will accept "microevolution" but deny "macroevolution" (whatever such a distinction means, if anything) - individuals who will accept what they see as "just" adaptation within populations but are still diehard creationists at heart. And then there are the "theistic evolutionists" - people who will accept that evolution is completely true but nonetheless insist that life was originally started by God; they posit that God acted as a sort of kickstart for evolution. In a sense, they are still a form of creationist, albeit a "weak creationist", since they still believe that life was created by a supernatural force and evolution proceeded from there. But there is another form of creationist, one that falls in between the last two categories. These are the individuals who will accept evolution in all cases except as it applies to humans. They believe humans to be God's "chosen" species (though, given the plethora of ailments we humans often suffer from, one might begin to wonder what benefit being chosen has, if any), and we were created in cutis by God as mentioned in the Bible and have remained the same ever since. This is a weaker form of theistic evolution (which itself is a weak form of creationism1!), and quite obviously, a case of special pleading.
All of these positions are untenable for a variety of reasons but it is the problems with this last position - that of the "evolution for all but humans" proponents (which I'll refer to as Humans-Only Creationism, or HOC, for simplification) - that I wish to focus on.
Being that those who hold such a view are accepting of the evidence for evolution in all cases except that pertaining to the evolutionary history of hominids, it is perhaps unexpected that evolutionary evidence of the hominid lineage would raise issues for this view point. Let us assume for a moment that humans are a special case - that they were created as is by God, and have remained unchanged since their genesis. What, then, would we make of the other hominid fossils that have been found? Since HOC makes the claim that humans have not evolved, then these fossils could only possibly be either fully "human" or fully "non-human" (or "fully ape", most creationists would claim), as any gradient between the two would indicate evolution. But this is problematic. Firstly, how would one determine which category any particular fossil specimen belonged to? Many fossils have traits that are "human-like" and also other traits that may be described as "ape-like". No one specimen has characteristics of only one or the other - they are an amalgamation of traits both human- and ape-like. Secondly, the record of hominid fossils does show a gradient from more "ape-like" to more "human-like" in many characteristics, and to claim that such a gradient does not exist is to outright deny observable fact.
Also, the "ape-like" hominids create problems for HOC. If they are not hominids, then what, exactly, are they? They are obviously more like humans than any extant primate. Are they supposed to be Gods "failed attempts" at creating humans? But if God is supposedly omnipotent, then how could this be? How could a perfect being create an imperfect creation? He would surely have gotten it correct on the first attempt. Anyone who subscribes to HOC has no choice to claim that God created them for a specific purpose. Why, then, did he create them so similar to humans?
HOC proponents are also guilty of doublethink. They freely admit to accepting evolution for all other species based on the overwhelming evidence in its favour. But in the same breath, they dismiss with a wave of the hand the idea that humans evolved - an idea which is based on the very same sort of evidence that they accept for other species! How one can hold these two beliefs at once and not succumb to crippling cognitive dissonance is beyond me.
When the evidence is examined, of course, the reality shows though - humans, like every other animal in existence, is the product of countless years of evolution.
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1) Perhaps we should call this idea "doubleweak creationism".
I would write a long, lengthy rebuttal to this video, but honestly, I have no idea what's going on in it. I see some really big numbers that have seemingly been pulled out of the air, repeated references to some sort of "linguistic law" and numerous claims that some "fact" or other has been "confirmed by science" but lacking any reference or sources...but none of it makes any kind of sense. It's sort of like sentences, ripe with nonsense, have been superglued together to make one giant ten minute long absurdity of cycloptian proportions.
In other words, overlapping gene pairs can be explained easily by a natural process. Two genes exist with reading frames shifted relative to one another, with one upstream from the other. The loss of a stop codon in the upstream gene results in this gene being extended into the region of the second gene where it ends at a stop codon. The result, then, is two genes which share a region of sequence. This has an important evolutionary consequence. The novel region is free to take on novel cellular functions. For the reasons stated above, the novel region is under fewer constraints. In fact, the creation of proteins de novo in this manner has likely played a very important part in viral evolution4. In many viruses, the novel protein in overlapping protein pairs are virulence factors or encode enzymes that allow the virus to escape host defence mechanisms. De novo creation of novel proteins by overlapping genes represents another mechanism by which novel "information" is added to the genome, something creationists love to deny is possible. 
