What Behe Actually Said

_{Barry Arrington

August 13, 2006

Intelligent Design}

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For those who are interested in what Professor Behe actually said in Dover (instead of the distortions of his testimony in Judge JonesÃ¢â‚¬â„¢ opinion), click on Ã¢â‚¬Å“more.Ã¢â‚¬ÂÃ‚Â [Thank you to tribune7 for sussing this out].

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Q. I just want to make a point clear. You said there were two examples where those who claim that irreducible complexity does not work or is not a valid explanation, they use experimental evidence, and that was the blood clotting system and the lac operon. How does the immunity system, is that experimental evidence or is that a theoretical claim?
A. No, this is mostly a theoretical claim. There is no experimental evidence to show that natural selection could have produced the immune system. And I think thatÃ¢â‚¬â„¢s a good example of the different views that people with different theoretical frameworks bring to the table.
If we could show the next slide. Professor Miller shows this slide from a reference that he cited by Kapitonov and Jurka, and he has titled Summary, Between 1996 and 2005, each element of the transposon hypothesis has been confirmed. He has this over this diagram.
But again, as I mentioned previously, whenever you see diagrams like this, weÃ¢â‚¬â„¢re talking about sequence data, comparison of protein, sequences, or gene sequences between organisms. And such data simply canÃ¢â‚¬â„¢t speak to the question of whether random

mutation and natural selection produced the complex systems that weÃ¢â‚¬â„¢re talking about.
So Professor Miller Ã¢â‚¬â€ so, in my view, this data does not even touch on the question. And yet Professor Miller offers as compelling evidence. And one more time, I view this as the difference between two people with two different expectations, two different theoretical frameworks, how they view the same data.
And IÃ¢â‚¬â„¢d like to take a little bit of time to explain why such studies do not impress me. And IÃ¢â‚¬â„¢ll do so by looking at one of the papers that Professor Doolittle Ã¢â‚¬â€ IÃ¢â‚¬â„¢m sorry, Professor Miller, thatÃ¢â‚¬â„¢s his name, cited in his presentation, Kapitonov and Jurka, that was published this year.
I just want to go through, and just kind of as a quick way to show why I am not persuaded by these types of studies. I want to excerpt some sentences from this study to show what I consider to be the speculative nature of such studies.
For example, in this excerpt, the authors say, something indicates that they may be important. This may indicate. It may be encoded. It might have been added. If so, it might have been derived. Alternatively, it might have been derived from a separate unknown transposon. It was probably lost. And we have a lot more of those, one more slide at least.
It says, we cannot exclude the possibility. In any case, the origin appears to be a culmination of earlier evolutionary processes. If so, this might have been altered. Again, without going into the detail of the article, I just wanted to emphasize those phrases to point out what I consider to be the very speculative nature of such papers.
HereÃ¢â‚¬â„¢s what I view to be the problem. The sequence of the proteins are there. The sequence of the genes are experimentally determined. And the question is, what do we make of that information? People like Professor Miller and the authors of this paper working from a Darwinian framework simply fit that data into their framework.
But to me, that data does not support their framework. It does not offer experimental evidence for that framework. TheyÃ¢â‚¬â„¢re simply assuming a background of Darwinian random mutation and natural selection and explaining it Ã¢â‚¬â€ or fitting it into that framework, but theyÃ¢â‚¬â„¢re not offering support for it.
Q. Dr. Behe, is there another paper that scientists point to for the support that the immune system can be explained by this Darwinian process?
A. Yes, there is. There is one more that I have to discuss. Here is a recent paper, again the year 2005, by Klein and Nikolaidis entitled The Descent of the Antibody-Based Immune System by Gradual Evolution. And on the next slide is an excerpt from the initial part of their discussion where they say, quote, According to a currently popular view, the Big Bang hypothesis, the adaptive immune system arose suddenly, within a relatively short time interval, in association with the postulated two rounds of genome-wide duplications.
So these people, Klein and Nikolaidis, are going to argue against what is the currently popular view among immunologists and people who study the immune system on how that system arose.
Q. And what is the Big Bang hypothesis thatÃ¢â‚¬â„¢s referred to here?
A. Well, thatÃ¢â‚¬â„¢s kind of a label that they put on to kind of indicate the fact that the immune system appears in one branch of animals, the vertebrates, and any obvious pre-cursors or functional parts of such a system do not appear to be obvious in other branches of animals.
So it seems like the immune system arose almost complete in conjunction with the branching of vertebrates from invertebrate.
Q. Do scientists acknowledge that or treat that as a problem for DarwinÃ¢â‚¬â„¢s theory?
A. Well, in my experience, no, nobody treats such a thing as a problem for DarwinÃ¢â‚¬â„¢s theory.
Q. Do you consider it a problem?
A. I certainly consider it a problem. But other scientists who think that Darwinian evolution simply is true donÃ¢â‚¬â„¢t consider much of anything to be a problem for their theory.
Q. Why do you consider it a problem?
A. Because the Ã¢â‚¬â€ as Darwin insisted, he insisted that adaptations had to arise by numerous successive slight modifications in a very gradual fashion. And this seems to go against the very gradual nature of his view.
Q. Now has this paper been held up by scientists as refuting claims against intelligent design?
A. Yes, it has. As a matter of fact, Professor Miller cited it in his expert report, although he didnÃ¢â‚¬â„¢t refer to it in his testimony. Additionally, I attended a meeting on evolution at Penn State in the summer of 2004 where one of the authors, Juan Kline, spoke on his work, and he interpreted it in those terms.
Q. Now we have some quotes, I believe, from this paper that you want to highlight?
A. Yes. Again, I want to pull out some excerpts from that paper just to show you why I regard this as speculative and unpersuasive. For example, they start with, by saying, quote, Here, we sketch out some of the changes and speculate how they may have come about. We argue that the origin only appears to be sudden. They talk about something as probably genuine.
It probably evolved. Probably would require a few substitutions. It might have the potential of signaling. It seems to possess. The motifs presumably needed. One can imagine that a limited number. It might have been relatively minor. Quote, The kind of experimental molecular evolution should nevertheless shed light on events that would otherwise remain hopelessly in the realm of mere speculation. TheyÃ¢â‚¬â„¢re talking about experiments that have yet to be done.
Next slide, I have even more such quotations. These factors are probably genuine. Nonetheless. They might have postdated. Nevertheless. Albeit. It seems. This might have been. These might represent. They might have been needed. This might have functioned. This might have. And this might have contributed.
So again, this is just a shorthand way of trying to convey that, when I read papers like this, I do not see any support for DarwinÃ¢â‚¬â„¢s theory. I read them as speculative and Ã¢â‚¬â€ but nonetheless, people who already do believe in DarwinÃ¢â‚¬â„¢s theory fit them into their own framework.
Q. Now Dr. Miller cited numerous papers in his testimony to support his claims on irreducible complexity, the type III secretory system, and so forth. Have you done a review of those papers and have some comments on them that you prepared slides for?
A. Yes, I did. I went through many of the papers that Professor Miller cited, as many as I could, and simply, as a shorthand way of trying to indicate or trying to convey why I donÃ¢â‚¬â„¢t regard any of them as persuasive, I simply did a search for the phrases, random mutation, which is abbreviated here in this column, RM, and the phrase, natural selection.
Random mutation, of course, and natural selection are the two elements of the Darwinian mechanism. That is what is at issue here. And so this is, you know, this is, of course, a crude and perhaps shorthand way, but nonetheless, I think this illustrates why I do not find any of these papers persuasive.
When I go through the papers that Professor Miller cited on the blood clotting cascade, Semba, et al, Robinson, et al, Jiang and Doolittle, there are no references to those phrases, random mutation and natural selection.
Q. Some of your indications on this slide, you have 0 with asterisks and some without. Is there a reason for that?
A. Yes. The papers that have asterisks, I scanned by eye. I read through them visually. Ones that do not have an asterisk, I was able to do a computer search for those phrases because they are on the web or in computer readable form. I have a number of other such tables.
On the next one are references that Professor Miller cited on the immune system. And again, none of these references contain either those phrases, random mutation and natural selection. There were a couple more references on the immune system that Professor Miller cited, and they didnÃ¢â‚¬â„¢t contain those phrases either.
In references for the bacterial flagellum and the type III secretory system, there was one paper by Hauch, a review in 1998 that did use the phrase natural selection. However, that phrase did not occur in the body of the paper. It was in the title of one of the references that Hauck listed.
And on the next slide, I think there are papers cited by Professor Miller on common descent of hemoglobin. And again, those phrases are not there. I think thereÃ¢â‚¬â„¢s another slide or two, if IÃ¢â‚¬â„¢m not mistaken. This is the one on what he described as molecular trees, Fitch and Margoliash, from 1967. And I didnÃ¢â‚¬â„¢t find the phrase there either. So again, this is a shorthand way of showing why I actually considered these off-the-point and unpersuasive.
Q. So all these papers that are being used to provide evidence for DarwinÃ¢â‚¬â„¢s theory of evolution, in particular, the mechanism evolution of natural selection, yet they donÃ¢â‚¬â„¢t mention random mutation or natural selection in the body of the works?
A. ThatÃ¢â‚¬â„¢s correct.
Q. Could you summarize the point then, Dr. Behe, that you are making with, referring to these studies and the comments you made about the speculative nature of some of these studies?
A. Yes. Again, much of these studies, in my view, are speculative. They assume a Darwinian framework. They do not demonstrate it. And certainly, you know, certainly scientists should be free to speculate whatever they want. You know, science usually starts with speculation, but it canÃ¢â‚¬â„¢t end with speculation.
And a person or, and especially a student, should be able to recognize and differentiate between speculation and actual data that actually supports a theory.

Q. Is this Ã¢â‚¬â€ so youÃ¢â‚¬â„¢ve done work in this area with the histone H4 and the molecular clock?
A. Yes, uh-huh. IÃ¢â‚¬â„¢ve written this commentary in 1990 in a journal called Trends in Biochemical Sciences, commenting on the work of somebody else who experimentally took an organism called yeast into the lab and altered its histone H4 and actually chopped off a couple amino acids at the beginning portion of that protein.
And when he looked, it seems that it didnÃ¢â‚¬â„¢t make any difference to the organism. The organism grew just as well without those mutations, which is surprising, which is not what you would expect if all of those residues were critical for the function of that protein, histone H4.
Later on, in the year 1996, I and a student of mine, Sema Agarwal, we were interested in this problem of histone H4 and molecular clock, and so we experimentally altered some amino acid residues into protein and changed them into different amino acids, with the expectation that these might destroy the function of the protein. But it turned out not to.
These positions, these amino acids could be substituted just fine, which is unexpected, and which kind of complicates our interpretation of the molecular clock hypothesis. So there are two complications; complications upon complications.
One, we would expect the number of mutations to accumulate with generation time, but it seems to accumulate, for some unknown reason, with absolute time. And the second is that, proteins accumulate mutations at different rates. We would expect that it would have to do with how vulnerable they are to mutations, and mutations might destroy the function of one protein that evolved slowly, but that is not experimentally supported.
Q. Now has this problem been discussed in the scientific literature?
A. Yes, this has been continuously discussed ever since the idea of the molecular clock hypothesis was first proposed in the early 1960Ã¢â‚¬â„¢s by two men named Emile Zuckerkandl and Linus Pauling. And here are a couple of papers which deal with the difficulties of the molecular clock hypothesis.
HereÃ¢â‚¬â„¢s a recent one, Gillooly, et al, published in the Proceedings in the National Academy of Sciences, entitled The Rate of DNA Evolution, Effects of Body Size and Temperature on the Molecular Clock. In this publication, they say that, in fact, the size of an organism and temperature can affect how fast or how slow this clock might tick.
Francisco Ayala has written on this frequently. HereÃ¢â‚¬â„¢s one from 1997. And I should say, Francisco Ayala is a very prominent evolutionary biologist. He wrote an article in 1997 entitled Vagaries of the Molecular Clock. And I think the title gets across the idea that there are questions with this hypothesis.
And in 1993, a researcher named Tomoka Ohta published an article in the Proceedings of the National Academy of Sciences entitled An Examination of the Generation-time Effect on Molecular Evolution in which she considers exactly that complication that the textbook Voet and Voet pointed out, this generation-time effect.
You know, why shouldnÃ¢â‚¬â„¢t organisms that reproduce more quickly accumulate more mutations. I have another slide just from one more recent paper. This paper by Drummond, et al, is entitled Why Highly Expressed Proteins Evolve Slowly. And itÃ¢â‚¬â„¢s referring to the sequence evolution that IÃ¢â‚¬â„¢ve been discussing.
It was published in the Proceedings of the National Academy of Sciences, and this was from an online version. This is so recent that I donÃ¢â‚¬â„¢t think it has yet appeared in print. The point I want to make with this is that, these people treat this question as a currently live question.
They start off by saying, a central problem in molecular evolution is why proteins evolve at different rates. So that question I was trying to illustrate with histone H4, why does one protein tick faster and another one tick more slowly, thatÃ¢â‚¬â„¢s still Ã¢â‚¬â€ that is still unknown.
And I think I will skip the rest of this slide and go to the next slide and just point out a couple words here. Drummond, et al, say, Surprisingly, the best indicator of a proteinÃ¢â‚¬â„¢s relative evolutionary rate is the expression level of the encoding gene.
The only point I want to make with this is that, they are reporting what is a surprise, what was not expected, which was not known, you know, 40 years ago, which has only been seen relatively recently. And they say, quote, We introduce a previously unexplored hypothesis, close quote.
And the point I want to emphasize is that, here in this paper published, you know, weeks ago, that they are exploring new hypotheses to try to understand why proteins have the sequences that they do.
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Comments

John A. You like to repeat that "Chance played no role whatsoever in either the origin or origins of life, its subsequent phylogeny or its present ontogeny which is all that remains." Did mass extinctions like the dinosaur happen by chance?idnet.com.au_{August 14, 2006
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Nick
Except that transposition occurs all the time, and diversity in immune receptors is positively selected for in a wide variety of critters. ItÃ¢â‚¬â„¢s not all that remarkable really.
We are not talking about a mere unremarkable transposition. We are taking about an alleged "initial integration event" which, "in one step, inserted both the RAG genes and the RSS sequences, and generated a rearranging antigen receptor." This is what I mean by a "hopeful monster" or "one big luck mutation." It has been noted that such arguments are no different than appeal to miracle. (abiogenesis for example)
The gene rearrangements that produced the modern VDJ system are mostly quite standard processes of duplication etc. For more detail see this 2000 review paper, also linked: http://www.jem.org/cgi/content/full/191/10/1631
I reviewed your paper. As you noted it was written in 2000, anyway it doesn't seem to give the detail you suggested. Note in the summary it states:
It remains to be pointed out that some of the most extensive changes that have occurred during the evolution of Ig and TCR loci cannot be explained by some combination of the operations shown in Fig 2. The conversion of "cluster" type loci to the "extended" form is not easily understood, nor is the huge variation in multiplicity of gene segments at different loci, or the manner in which, for some loci, gene segments were first flipped into an opposite transcriptional orientation.
What we IDists are interested in is how you cross the huge information barriers necessary to construct complex and IC systems. Again, pointing to "deep" homologies and "hopeful monsters" only strengthens the ID case. If there is an explanation for how these information barriers are crossed you still have not demonstrated it.Jehu_{August 14, 2006
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Chance played no role whatsoever in either the origin or origins of life, its subsequent phylogeny or its present ontogeny which is all that remains. "Neither in the one nor in the other is there room for chance." Leo Berg, Nomogenesis, page 134 The idea of a predetermined (prescribed) evolution is not new and can be traced back to Bateson: "Finally, Bateson likewise (1914, page 640) inclines to the view that the entire process of evolution may be regarded as an 'unpacking of an original complex which contained within itself the whole range of diversity which living things present.'" Leo Berg, Nomogenesis, page 359 Intelligent Design by elements far beyond our comprehension, in my view, is not an inference, but a mandatory starting point without which nothing in the inanimate or animate world will ever make any sense. Phylogeny is the perfect model for phylogeny. Both have always proceeded on the basis of contained initial information and the only role for the environment was that of providing a stimulus. The usual stimulus for the development of the egg is penetration by the sperm which can be substituted for with a needle. The male haploid nucleus is quite unecessary and for many forms it provides no information anyway, serving only as an activating agent. These are not surmises but experimentally verified conclusions. I believe that the spermatazoon initially was an activator only, which later, with the several independent inventions of sexual reproduction, became a contributor of genetic information. With mandatory sexual reproduction, all creative evolution ceased which is why it cannot be demonstrated today. Sexual reproduction, allelic mutation and natural selection are all conservative anti-evolutionary devices. Accordingly, Mendelian genetics had nothing to with with creative evolution either. All it can manage is the creation of subspecies and varieties neither of which are incipient species. Bateson realized this too as I presented elsewhere here at Uncommon Descent as well as in published hard copy. The truth lies elsewhere and I think it lies in the Semi-meiotic hypothesis (SMH) which still awaits testing with suitable material. Like all hypotheses it remains viable until found to be inadequate. Don't expect Darwinian laboratories to undertake these experiments as they quit testing their own hypothesis decades ago. Actually Darwinism has never been an experimental science anyway and to that extent Darwinians are not scientists! Certainly none of their recent spokespersons are or were, Richard Dawkins, Stephen J. Gould and Ernst Mayr, all of whom retired early, became glued to their endowed chairs and dedicated the rest of their lives to book after book extolling the atheist Darwinian fairy tale. So much for Darwinism. It is hard to believe isn't it? I love it so! "A past evolution is undeniable, a present evolution undemonstrable." John A. DavisonJohn A. Davison_{August 14, 2006
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Since I donÃ¢â‚¬â„¢t have PhD it is possible I have misunderstood the explanation. However, as I read it now it seems like a Ã¢â‚¬Å“hopeful monsterÃ¢â‚¬Â scenerio depending on one big lucky muation. Except that transposition occurs all the time, and diversity in immune receptors is positively selected for in a wide variety of critters. It's not all that remarkable really. The gene rearrangements that produced the modern VDJ system are mostly quite standard processes of duplication etc. For more detail see this 2000 review paper, also linked: http://www.jem.org/cgi/content/full/191/10/1631 ...not completely up to date but quite useful. You were quoting Matt Inlay's 2002 essay, note that since then they have found the homologs of the ancestral receptor and the hypothesized transposon, which were a "mystery" in 2002. Surely the evolutionary immunologists deserve some credit for that. Regarding the various questions about how to test your alternative explanation, a design model that somehow involves the transposon the evolutionary biologists predicted and discovered -- I could give you my thoughts, but you have to actually present a design model first. But once you've reached this point, you are now arguing something different: "ID can explain the data too" -- which concede that evolution already provided an answer, which is exactly what Behe denied.Nickm_{August 14, 2006
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By Jehu: "Since I donÃ¢â‚¬â„¢t have PhD it is possible I have misunderstood the explanation. However, as I read it now it seems like a Ã¢â‚¬Å“hopeful monsterÃ¢â‚¬Â scenerio depending on one big lucky muation." I think some of the people here may have some misconceptions about how science proceeds. The transposon hypothesis began in 1979 when the Tonegawa lab sequenced the immunoglobulin genes and found sequences that resembled the ends of transposons. They asked the question of whether or not the V(D)J recombination system may have arisen from a system similar to transposons. If the V(D)J recombination system evolved from a transposon, what features would be expect to find in the V(D)J recombination system? The subsequent experiments in the last 25 years on that issue were inspired by that question. Think to yourself, what would we expect to find? Well, at that point, the RAG genes hadn't been discovered yet, so one prediction based on that model was that the RAG genes were transposases. When the RAG genes were discovered, their genomic organization was very similar to transposons (two genes, tightly clustered, no introns). A few years later, it was discovered that RAG genes had transposase activity, first in the test tube, then evidence was found in organisms. Remember, Behe specifically mentioned the RAG genes and V(D)J recombination in Darwin's Black Box. He said that components of IC systems would not be found outside of the IC system (unless they evolved FROM the IC system, as is argued for the Type III secretory systems). However, in contrast to Behe's predictions, we found RAG genes outside of mammals, in organisms that have nothing that resembles an adaptive immune system. Now does this satify Behe's requirements for an answer? Probably not, nor will it ever. But every other immunologist considers the transposon origin model essentially proven precisely because of the wealth of evidence that's been accumulating for the last 25 years on it. There's been no result that seriously undermines this model. It may help to think of this like a murder investigation. We have a prime suspect, and we hypothesize that he is the killer. We ask, what would the evidence be if our prime suspect was the killer? We find that the killer was left handed, between 6'1" and 6'4", was blood type O, and had blonde hair. We find that the prime suspect had all those features. Certainly there are many people out there that would fit that description, but then we find the suspect had no alibi, and that he would have profitted tremendously by that person's death. Again, more and more evidence points to him. We then find that he owns a gun, and the bullet drawn from the victim matches his gun. Furthermore, ballistics shows that the bullet has the same markings as a bullet fired from the suspect's gun. What we see in this example is a steady accumulation of evidence all pointing to a single conclusion, that the suspect is the killer. Would a jury insist on a moment-by-moment account of the suspects exact whereabouts the night of the murder? Would they demand proof that the suspect fired that gun on that night? There are a million ways a jury can nit-pick the case, and a defense lawyer can invent alternative theories with no evidence for them whatsoever, but when is enough enough? The community of immunologists has been following this case for a long time, and they all agree, the transposon model is without doubt the current, best explanation for the origin of the V(D)J recombination system. Of course, all the evidence has already been linked to, again and again. It's there if anyone is interested in looking at it and discussing it.minlay_{August 14, 2006
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Andrea and/or NickM No answer for my question in comment 21 about what tests were performed to discriminate between chance and design in the series of mutations leading to the immune system component in question? I didn't think you'd be able to point to any testing in that regard. I was hoping one of you would at least show enough intellectual honesty to admit it. There's still time. I'll presume you missed the question. And since this thread is about what Behe actually said I'll point out that Behe accepts descent from one or a few common ancestors as a reasonable position. He may harbor some measure of doubt but it's not a lot. I too harbor some measure of doubt but it's very little. The fossil record, molecular homology, common genetic code, and the observation that life always comes from life, are enough to convince me beyond reasonable doubt that common ancestry is true. But it's an inference and as such there must always remain some measure of uncertainty. Design is also an inference and for me there is more doubt about it but I think it's the best explanation for the origin of the first cell using DNA and ribosomes. The chance formation of digital program and data code that drives a protein assembly machine like a factory robotics system is just too much for me to swallow without a plausible explanation for how it was possible. If that can be demonstrated I'm willing to concede everything that followed was driven by chance as well. Absent such demonstration, design of the first cell by an unknown agent or agency, remains a live possibility. And if the first cell was designed it also remains a live possibility that the original genome was not simple but rather very complex and contained all the information needed to diversify along a more or less preset path with chance playing little if any role in the diversification much as a fertilized egg cell has all the information to diversify into all the myriad different cells and organization that makes a human being.DaveScot_{August 14, 2006
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My last post had some HTML errors and puts my own words in blockquotes. My apologies for any confusion.Jehu_{August 14, 2006
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Nick
See the links and references for moreÃ¢â‚¬Â¦if you dare. So far I have seen very little evidence that you guys follow links to uncomfortable scientific evidence.
Well Nick, I followed your link, and I was immediately informed of the following.
"hundreds of PhD scientists have devoted their careers to working out how and why the immune system evolve"
Wow. That is really amazing. Here is the summary I was given of what those "hundreds of PhD scientists" of come up with for the evolution of the immunoglobulin activation/secretion pathway:
(1)It begins first with an innate membrane-bound receptor that can induce the transcription and release of antimicrobial peptides upon interaction with a specific foreign antigen (such as LPS). (2)A mutation results in an alternative mRNA splice variant that directs the synthesis of a secreted form, providing a selectable advantage. (3)Finally, the ability to generate a diverse repertoire of antigen-receptors through gene rearrangement evolves. I can barely make spaghetti in three easy steps but thanks to hundreds of PhD's devoting their careers the immunoglobulin activation/secretion pathway can evolve in three steps. Of course further detail lets me know that step (3) pretty much is one step.
Assuming that a non-rearranging antibody-like gene is beneficial, two important components had to appear during the evolution of antibody diversity: the signal sequences and the RAG genes. Their origin is indeed a mystery. Ã¢â‚¬Â¦ The initial integration event, in one step, inserted both the RAG genes and the RSS sequences, and generated a rearranging antigen receptor.
Since I don't have PhD it is possible I have misunderstood the explanation. However, as I read it now it seems like a "hopeful monster" scenerio depending on one big lucky muation. As I understand it, the basis of Intelligent Design is the challagne that the complexity in life cannot be achieved by RM+NS. When ID encounters certain complex systems, especially IC systems, it sees an information problem that cannot be overcome by RM+NS. Therefore, pointing to "deep" homologies or phylogenic difference does not overcome the objection that ID raises. Additionally, appeals to "hopeful monsters" and big lucky mutations only strengthens the ID objection.Jehu_{August 14, 2006
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Joseph: "Andrea here is YOUR chance- tell us how to objectively test common descent, as in chimps and humans share a common ancestor." How about letting a self-proclaimed creationist answer your question: http://members.iinet.net.au/~sejones/cmnctsry.html In particular, please check out the sections "Vitamin C pseudogene" and "Human-Ape chromosome map (karyotype) comparison".ofro_{August 14, 2006
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Oh, so you guys *do* accept the transposon hypothesis? You accept that it is testable and has passed the tests I linked to? I guess the scientific community *does* have an answer then, and Behe was wrong about "no answers." You have no problem with common ancestry? Tell that to Joseph of comment #27. Or have a look at Pandas: "Design proponents have a realistic and more cautious approach to the use of homologies. They regard organisms which show great structural differences, such as starfish and chimpanzees, as having no common ancestry." (p. 127) "This is precisely why a book that questions the Darwinian notion of common descent is so necessary. By presenting a reasonable alternative to evolution in this second sense (i.e., common ancestry), Pandas helps students learn to work with multiple perspectives, to distinguish those perspectives from facts, and to guard themselves against the illusion of knowledge." (p. 156)Nickm_{August 14, 2006
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Tribune7 said (comment #6) -- "Nick -- The threads about Jones concern the legal aspects of the case." Andrea replied (comment #8) -- "I guess that explains why neither Nick nor I have been able to discuss the actual published evidence, and no one seems to actually even care to look at it." Tribune7 replied (comment #11) -- "Maybe if you hadnÃ¢â‚¬â„¢t mischaracterized BeheÃ¢â‚¬â„¢s testimoney you might have been taken more seriously for a serious discussion." The reason why Darwinists have been mischaracterizing Behe's testimony is that they are more interested in defending Judge Jones and the Dover decision than they are in discussing the science. I have yet to see a Darwinist concede that Judge Jones could possibly do anything wrong. The article "Traipsing into breathtaking inanity" on my blog lists many flaws in the Dover decision and court proceedings, and that article does not even get into discussing the scientific issues -- see http://im-from-missouri.blogspot.com/2006/04/traipsing-into-breathtaking-inanity.html My blog also has about ten other articles that denounce Judge Jones.Larry Fafarman_{August 14, 2006
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Andrea here is YOUR chance- tell us how to objectively test common descent, as in chimps and humans share a common ancestor. It isn't that people deny it- It is that people deny there is a way to objectively test the premise and THAT is minus any underlying mechanism. And if you want to talk about nutty positions check out evolution #6- The meanings of evolution, from "Darwinism, Design and Public Education": 1. Change over time; history of nature; any sequence of events in nature 2. Changes in the frequencies of alleles in the gene pool of a population 3. Limited common descent: the idea that particular groups of organisms have descended from a common ancestor. 4. The mechanisms responsible for the change required to produce limited descent with modification, chiefly natural selection acting on random variations or mutations. 5. Universal common descent: the idea that all organisms have descended from a single common ancestor. 6. Ã¢â‚¬Å“Blind watchmakerÃ¢â‚¬Â thesis: the idea that all organisms have descended from common ancestors solely through an unguided, unintelligent, purposeless, material processes such as natural selection acting on random variations or mutations; that the mechanisms of natural selection, random variation and mutation, and perhaps other similarly naturalistic mechanisms, are completely sufficient to account for the appearance of design in living organisms. Absolutely nuts especially given what we do know...Joseph_{August 14, 2006
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What I absolutely fail to get is how it is possible for people like Nick and Andrea to persist in their incapacity to understand that in fact ID has NO PROBLEM with evolution and even common descent. Tina, I suspect it's because recurrently one finds statements like this in ID books and at ID web sites: https://uncommondescent.com/index.php/archives/1446 in which someone claiming that **there is no evidence for speciation** is quoted approvingly by Wells. And when in that thread I pointed out that in fact even the YECs at AiG accept that speciation occurred, I was accused of "ad hominem" (?), and of "changing the subject". No one in that thread has pitched in to say that in fact the claim is, by any reasonable interpretation, nonsense. And then there is the fact that most of the ID experts who testified in Kansas denied common descent, and that whenever a new transitional fossil is publicized, ID sites are quick to point out that they are not really "transitional", but "chimeric", and so on. I understand that ID is a Big Tent, but its advocates can't claim collective immunity from criticism of nutty positions, as long as they are admitted under the tent. At the very least, letting nutty positions in without any sign of internal criticism is a bad indicator as far as scientific rigor goes.Andrea_{August 14, 2006
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If heÃ¢â‚¬â„¢s not claiming (with Andrea) that Behe is a buffoon who gets his scientific info from the NY Times This is a blatant mischaracterization (to use a mild expression) of what I, and Nick, said.
Well, then just be glad I didn\'t allow some of Nick Matzke\'s more offensive comments through the UD filters. I had already read the page on www.ncseweb.org 2 days ago and my reaction was along the lines of \"that\'s it??\". Considering the tone of your comments I was expecting much more than a game of connect the dots via imagination. Then again, you\'ve already argued \"much more\" is superfluous... As for the main question, there are probably 6 major views: 1. Evolved via RM+NS. 2. The RAG genes descended from a transposon via an intelligent process like is suggested with PEH, latent library, etc. 3. Theistic evolution--not random at all but prescribed. 4. Tinkering designer. 5. Designer reuse. 6. Self-analysis and modification program built into DNA...somewhere. Miss anything? I doubt many here would support 1, 3, or 4. Either 2 or 5 is fine with me...6 was just thrown into the list as an act of whimsy. Now everyone can argue about which interpretation is best. As for 5: Similarities in different systems are to be expected from an Intelligent Designer when similar functionality design goals are the target. As for RAG1-RAG2 homologs serving a non-immune function in sea urchins...heck, just this last week I was coding some new functionality and borrowed large chunks of code from a function that had a different purpose. Some of my functions are purposely designed to be general purpose so they can be reused all over the place for different types of functionality. On a side note, it would be nice if Behe had the time to respond personally (what is he up to nowadays, anyway?).Patrick_{August 14, 2006
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Tina, they also persist with the \"Tinkering god\" canard. They seem to be unable to grasp the idea that everything may have been preprogrammed at the very start to unfold at given intervals. With the codes wrapped within codes which we are observing at the molecular level, it just seems silly to me that intelligent people would opt for the primitive notion that only external unguided pressures led to the complexity we see. C\'mon folks, we have new data.Scott_{August 14, 2006
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What I absolutely fail to get is how it is possible for people like Nick and Andrea to persist in their incapacity to understand that in fact ID has NO PROBLEM with evolution and even common descent. How is it possible that obviously intelligent people continue to think that every snippet of evidence that change took place is evidence that it took place via RM+NS? Help help help me to understand this bizarre twist in the debate...tinabrewer_{August 14, 2006
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NickM: Only creationists think it is an actual argument to highlight words like Ã¢â‚¬Å“probablyÃ¢â‚¬Â in scientific articles, because they donÃ¢â‚¬â„¢t realize that scientists habitually use tentative language in all their work. Only true followers of dogma would accept such words as authoratative truth. Perhaps if people like NickM were as tentative about the dogma he is pushing the world could enjoy OPEN discussions as to the reality of our existence- ie what science should be attempting to answer. NickM: So far I have seen very little evidence that you guys follow links to uncomfortable scientific evidence. So far we have seen little evidence that you EVER plan to substantiate your claims. Does NickM even understand the debate? Or is he one of the perpetrators of the myth that IC = "it couldn't have evolved" myth? To NickM- Do you realize that IC is an argument against the blind watchmaker (ie unintelligent, blind/undirected (non-goel oriented) processes) and NOT an argument against evolution? (yes or no) NickM: No one at UD has even tried to answer this question yet, even though real science is about testing hypotheses, and this discovery was a dramatic confirmation of the evolutionary model. Tell us NickM how would one test the hypothesis that the bacterial flagellum "evolved" via some blind watchmaker-type process from a population (of bacteria) in which not one bacterium had such a structure? Here is your chance but my bet is you either won't accept the challenge or you will attempt to bluff your way through it. To this day I kick myself for not going to the "Kitzmiller" fiasco...Joseph_{August 14, 2006
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NickM and/or Andrea I don't dispute descent with modification from one or a few common ancestors. My bone of contention is whether or not it was entirely accidental or proceeded (more or less) by design. I believe the evidence we have so far warrants a design inference. In this regard I can't seem to get an answer to a certain question out of anyone who believes chance and necessity drove the entire process from the beginning to present. The question: What tests were performed to determine whether the series of mutations that led to the immune system component in question came about by chance or design? Silence will be taken to mean no such tests were performed and the presumption of chance is nothing but philosophical/areligous dogma rearing its ugly head in what should be objective scientific inquiry.DaveScot_{August 14, 2006
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If heÃ¢â‚¬â„¢s not claiming (with Andrea) that Behe is a buffoon who gets his scientific info from the NY Times This is a blatant mischaracterization (to use a mild expression) of what I, and Nick, said . Anyone reading the original thread can verify this is not true. It doesn't really help your cause to keep insist in this silly accusation.Andrea_{August 14, 2006
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Nick, As an expert on the case, perhaps you could tell us, or at least provide a link to (I promise I will follow it) a clear explanation of where exactly the 58 articles, etc show how *RM & MS* gave rise to the immune system. This is a great opportunity for you as a member of the NCSE to educate the public on this matter. As I am sure you are aware, this is the point Behe has been making all along. Thanks, antg PS I and probably most others here have no problem with RAG genes descending from a transposon. Again as I am sure you are aware, this is not the point in question.antg_{August 14, 2006
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OK, Sal, why don't you tell me why the scientists suspected that a transposon homologous to RAG should exist? The only reason anyone had to suspected its existence is that it was a direct implication of the evolutionary hypothesis that RAG genes descended from a transposon. No one at UD has even tried to answer this question yet, even though real science is about testing hypotheses, and this discovery was a dramatic confirmation of the evolutionary model.Nickm_{August 14, 2006
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Nick Matzke wrote: So far I have seen very little evidence that you guys follow links to uncomfortable scientific evidence.
Kind of hard to see evidence if you shut your eyes to it, Nick. I refuted your repeated equivocations. Phyglogeny does not automatically imply Darwinism, and further Behe is not averse to a phylogeny. Let me mark this as at least the 3rd time this has been brought to your attention and you've repeated the equivocation. Is that the way you do business for NCSE?scordova_{August 13, 2006
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Is anyone else tired of Nick's arrogance? His absurd statements are just too much. If he's not claiming (with Andrea) that Behe is a buffoon who gets his scientific info from the NY Times, he's making silly comments like this. Too bad his link doesn't even begin to answer the question asked! Of course, he has no evidence that natural selection caused transpons to become RAGs. But, he sure can point to the NCSE's "battle plan" against Behe with claims that A, B, and C maybe, might have, could have, possibly evolved in this manner in this particular possible pathway. Reading through the information, links, papers, I guess close is good enough for horsehoes AND science. Well NeoDarwinian views of science, at least,JasonTheGreek_{August 13, 2006
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And that is a philosophical question. In other words, you don't have a rebuttal to my point. The scientific Ã¢â‚¬â€ and relevant Ã¢â‚¬â€ one is how did natural selection cause transposons to become RAGs? Lucky for you, I layed out the basics here: http://www2.ncseweb.org/kvd/exhibits/immune/immune_evo_annotated_bib.html#sci See the links and references for more...if you dare. So far I have seen very little evidence that you guys follow links to uncomfortable scientific evidence.Nickm_{August 13, 2006
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We can debate these scientific issues until doomsday, but the fact will remain that Judge Jones violated Rule 803(18) of the Federal Rules of Evidence Larry, good point and good to get us back on topic.tribune7_{August 13, 2006
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Why, apart from the transposon model, should transposon homologs to the RAG genes even exist? And that is a philosophical question. The scientific -- and relevant -- one is how did natural selection cause transposons to become RAGs? Only creationists think it is an actual argument to highlight words like Ã¢â‚¬Å“probablyÃ¢â‚¬Â It's not an argument. It's an answer :-) Only an atheist could think otherwisetribune7_{August 13, 2006
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We can debate these scientific issues until doomsday, but the fact will remain that Judge Jones violated Rule 803(18) of the Federal Rules of Evidence - see https://uncommondescent.com/index.php/archives/1443#comment-53130 As Sir Thomas More said in the play "A Man for All Seasons," "The world must construe according to its wits. This court must construe according to the law." Also, this debate over these complex, contentious, and esoteric scientific questions shows the problems of trying to have such questions decided by a court of law. I feel that the courts should not even attempt to decide such questions unless absolutely necessary for deciding a case, and it was not absolutely necessary in Kitzmiller v. Dover. Judge Jones turned a deaf ear to 85 scientists who filed an amicus brief that urged him to refrain from ruling on the scientific merits of ID and irreducible complexity -- this brief said,
. . . . the scientific theory of intelligent design should not be stigmatized by the courts as less scientific than competing theories . . . . .litigation should not usurp the laboratory or scientific journals as the venue where scientific disputes are resolved. Doubts as to whether a theory adequately explains the evidence should be resolved by scientific debate, not by court rulings. . . . . . Whether or not intelligent design is adopted as an explanation for biological origins, science benefits from the competition of alternate hypotheses. Amici see great value to design theory simply because it forces scientists to confront evidence which conflicts with the Neo-Darwinian paradigm . . . . . -- from http://www2.ncseweb.org/kvd/all_legal/2005-10_amicus_briefs/2005-10-03_DI_amicus_biologists.pdf
Larry Fafarman_{August 13, 2006
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I guess that explains why neither Nick nor I have been able to discuss . . . Maybe if you hadn't mischaracterized Behe's testimoney you might have been taken more seriously for a serious discussion.tribune7_{August 13, 2006
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Another thing: Ã¢â‚¬Å“probablyÃ¢â‚¬Â, Ã¢â‚¬Å“mightÃ¢â‚¬Â Ã¢â‚¬Å“it seemsÃ¢â‚¬Â Ã¢â‚¬Å“one can imagineÃ¢â‚¬Â, Ã¢â‚¬Å“shouldÃ¢â‚¬Â are not answers. Only creationists think it is an actual argument to highlight words like "probably" in scientific articles, because they don't realize that scientists habitually use tentative language in all their work. Deal with the data. Why, apart from the transposon model, should transposon homologs to the RAG genes even exist? Scientists were speculating about the existence of these homologs for years before they were finally discovered in 2005. The only reason scientists looked for those homologs at all was that the transposon hypothesis said that the RAG genes were descended from a transposon. The evolutionary hypothesis is the only reason anyone thought to look for them.Nickm_{August 13, 2006
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Re: Friend of Richard Dawkins interviewed....... Sorry about posting here but I cannot find a contact email for your website. In New Zealand last weekend we had and ID basher guy on National Radio who is friends with Richard Dawkins. The audio interview is here: http://www.radionz.co.nz/audio/national/sat/robyn_williamsRobo_{August 13, 2006
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