Study Suggests Genome Instability Hotspots 72
Dr. Eggman writes "Ars Technica reports on a new study that suggests not only that certain areas of the mouse genome undergo more changes, but that changes to those areas are more tolerable by the organism than changes in other areas. Recently published in Nature Genetics, the study examined the certain copy number variations of the C57Bl/6 strain in mice that have been diverging for less than 1,000 generations. The results were a surprising number of variations. While the study does not address it, Ars Technica goes on to recount suggestions that genomes evolved to the point where they work well with evolution."
heh (Score:3, Insightful)
ya think?
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An extreme example of segments of DNA mutating faster than the rest comes from the mammalian immune system. Picture this: a mouse has less than 100k genes, but can make more than a million different antibodies. How? Each of the millions of B lymphocytes circulating in the bloodstream can only make one antibody, just one amino acid sequence. When the mouse is attacked by a particular disease, almost all of them will be useless against the disease. But the few that display antibodies that have any sort of ability to bind the disease do so, and this triggers those cells to undergo rapid mitosis. This produces many clones that can attack the disease; however, they're not exact clones. The gene that codes for the antibody has "C" (constant) regions and a "V" (variable) regions. Each antibody uses two identical "heavy" regions and two identical "light" regions. There are three parts of the "heavy" variable region -- VH, DH, and JH -- while there are two for the "light" variable region -- VL and JL. A molecule called AID changes a cytosine to a uracil, which isn't normally found in DNA. The body's DNA repair mechanism attempts to correct it, changing the gene in the process. There are about 50 possibilities for VH, 23 for DH, 6 for JH, 57 for VL, and 9 for JL. So, doing the math, you come out to a staggering 3 1/2 million antibody possibilities, all thanks to the extremely rapid evolution of the V regions. The more effectively the B lymphocite binds with the pathogen, the more its reproduction is activated, and the more copies of itself -- both identical and with slightly changed V regions -- it makes. This whole process is called "somatic hypermutation", and we couldn't survive without it.
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But I can't find any mention of the term "somatic hypermutation" in the Bible at all. Did they call it something else back then?
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What the article was talkin about in this regard is that a genome will tend to evolve in such a way that mutation rates will be at a good rate for the organism.
Indeed. Which is kind of related to this previous study Rate of Evolution Metrics Observed [slashdot.org] which showed that the optimum rate of evolution varied between small fast reproducing animals and larger slower reproducing ones.
What this adds is the news (or further evidence if it was already known) that the optimal rate might even vary across differ
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The article summary is poor, the real story i
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That's a bit over-interpreted, IMHO (Score:5, Interesting)
What this really says is that the genome became, more or less, fault-tolerant. The ability to evolve really came out of that.
For starters, there is no part of the genome or ribosomes or whatever that actually produces mutations. On the contrary, most of the complexity in your cells is to prevent mutations, to the best of possibilities. It's the only way to have a coherent organism made of gazillions of cells. You don't want a cell in your palm to think it's supposed to grow into a nose, for example. And you really don't want cells to just start divided uncontrolled.
And you or the mouse have layers upon layers of defenses against that. The very reason why we're DNA based instead of RNA is to allow repairing single-strand mutations. But it goes on from there.
The very fact that you age is, pretty much, a defense against cancer: cells have a maximum division number counter, based on what tumor size still likely wouldn't kill you. (Hence also why larger species tend to live longer: they get a bigger limit there.) When more and more cells have reached that limit, then more and more damage can't be repaired, and you discover the fun of old age. And then you die.
Etc.
At any rate, the major thing is: there is no part in the genome that says you should evolve. Read: mutate. It actually tries to prevent mutations, hence evolution.
But mutations happen anyway, and some will happen in the sperm or eggs, or the first stages of embryo formation. You can't 100% prevent those. They _will_ happen. And the choices from there are basically two: either the result can still live with that mutation, or it dies.
Hence what they discovered here: natural selection favours the kind of genome that can tolerate mutations when they happen anyway. A species where the slightest change results in death will be at a disadvantage, compared to a species where more individuals survive even with mutations.
Sure, in the long term that also means being to evolve and cope with environment changes. No doubt. But I think there's a far stronger short-term pressure to achieve the same result. And most likely that's really what we're seeing there.
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Is that a fact? I thought that big species die older, because their cells devide less often. So instead of having a bigger counter, they just count slower.
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That's true more or less by definition, but I think you're overlooking something simple. A more complex organism has more opportunities for nonfatal mutations. That is, Mycoplasm genitalium, probably the simplest known bacterium, is extremely vulnerable to deleterious mutations. If it loses a gene that codes for a vital self-component, odds are it hasn't got a backup process fo
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I wouldn't be surprised if this leads to life expectancy remaining stable despite ever-increasing medical technology. The more we are able to cure disease, t
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On top of that... (Score:2)
This is about as amazing as getting a group of people who roll dice
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I used to think the same way about it but the more I looked into it the more I realized that there is a way for species to regulate their evolution in a way. Genetic repair mechanisms to be exact. They have evolved to have some level of accuracy; this is different depending on what species you ar
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It doesn't mean anything. Talking about things being more or less "compatible with evolution" is just insane raving. Let me make it real simple: The living things which exist today exist because they are able to exist, and they will continue to exist because they are able to continue to exist. If that sounds tautological, that's because it is.
Evolution is simply the elimination of organisms which, under current conditions, cannot survive. Clearly any living thing must be "compatible with evolution" becaus
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"Strength" is an illusion created by people who think they have an idea of how things should be. I would say that they have developed a sense of blasphemous hubris, that they think their ideas for the world are superior to the ideas of the creator.
I believe in freedom, and I love that we keep finding evidence to support it as a basic law of the universe, written
That much is obvious, BUT... (Score:2)
The question for me is... WHERE is that information stored? In another part of the DNA? If so, it becomes metaprogramming. Somewhere else? If so, there's a new type of DNA (unless RNA etc. qualify as that; I'm no geneticist, admittedly).
The Next Step (Score:5, Interesting)
I think a fascinating next step would be to see if, statistically speaking, viruses and transposons were channeled into jumping into these "safer to change" hotspots rather than other, more fragile areas of the genome.
It would seem to make some sense, given all the potential for genomic havok inherent in viruses and transposons' tendency toward hopping into the middle of genes.
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I find it strange that organisms would allow *any* viruses etc. to tinker with its DNA. But I suppose it may spend more energy to defend the sensitive areas such that those areas that are more flexible to mutations are not as well protected; meaning they get hit more. Its like armor that pro
Re:The Next Step (Score:5, Informative)
That's kinda what viruses do. The virus by itself cannot reproduce (that's why it's normally not considered to be 'alive') - it has to hijack a cell's reproduction machinery to do the reproducing for it. In order to hijack the cell, it inserts its own viral DNA (or RNA - depends on the virus) into the cell's genomic DNA, and reprograms the cell to make more viruses.
Often, if the cell doesn't die from the infection, it passes on the viral genes as well when the cell reproduces. Our own human genome has a significant amount of viral DNA in it; most of it has been inactivated, but we still produce some viral proteins in very small amounts (reverse transcriptase for instance). I once heard the estimate that a full 15% of our genome has viral origins, but cannot find any reference to verify this claim at the moment - take it with a large grain of salt.
Now, cells do have several mechanisms that they use to defend against viral attacks. Most notably, restriction endonucleases. These are enzymes that chop up the DNA at certain sites. We use these enzymes all the time in genetics work. If you've seen images of agarose or acrylamide gels with patterns of lines on them, that's usually DNA that's been chopped into pieces by some of these endonucleases, and then separated by size. Restriction endonucleases are commonly found in bacteria, but can also be found in lower eukaryotes like yeasts.
Another method for defending against viral attacks is RNAses (enzymes that chew up RNA). This primarily works against viruses that use RNA as their genetic material. There's also the trick of marking your own genes with methyl groups so that you can tell the difference between it and foreign DNA, (if it's not marked, destroy it). Eukaryotes typically destroy any DNA found in the cytoplasm. So yeah, the cell does have several methods to defend against viral attack.
But I suppose it may spend more energy to defend the sensitive areas such that those areas that are more flexible to mutations are not as well protected; meaning they get hit more.
Once the virus genes have been inserted, removing them is quite difficult. Generally, viruses don't have a specific site that they insert to either, it's typically inserted at random. The reason that our own genes don't get significantly interrupted is that the majority of our genome doesn't code for anything; viruses insert themselves into areas we aren't using anyhow.
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(I've asked this in another spot, so pardon my own private dupe - cue b52 song.)
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But this is NOT the only possible mechanism.
Re:The Next Step (Score:5, Informative)
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I think a fascinating next step would be to see if, statistically speaking, viruses and transposons were channeled into jumping into these "safer to change" hotspots rather than other, more fragile areas of the genome.
"Duh."
If a retrovirus inserted itself into a part of the genome which immediately stopped the life functions of a cell, then the cell would die and the retrovirus would die. Thus, the only retroviruses which survive are those which do not cause immediate death of the host cell. There's n
Genome Hotspots (Score:5, Informative)
For very highly conserved genes such as the homeobox sequences, the degree of conservation is enormous. Nearly everything has the homeobox -or 'hox' sequence, and the sequence itself hasn't changed significantly (in comparison to most other genes). tRNA sequences as well don't change significantly; neither do ribosomal genes. Some stuff you simply can't change without experiencing lethal (or at least highly detrimental) results.
Other regions such as non-coding regions, and introns to a lesser extent, can be mutated significantly without any change to the phenotype of the organism. In fact, this is what a lot of DNA fingerprinting is based on - big variations in sequence lengths and other polymorphisms between individuals. These variations don't occur frequently enough within coding sequences to be of any use in identification. Rather, they check the non-coding areas and other mutational hotspots for differences. Conversely, changes in the protein-coding regions can be used to determine the relatedness between species (say, human and chimp differences, or rat and mouse) on a much longer scale.
Now, having said that, there are always exceptions. Some organisms have entirely novel mutation patterns. The influenza virus (admittedly, not an organism in the traditional sense) mutates almost exclusively in the coding areas of its envelope proteins. Even stranger, only 1 strain of the virus seems to survive every year to propagate the next. (See the 2001 article by Bull and Wichman entitled "Applied Evolution" in the journal 'Annual Review of Ecological Systems".)
Basically, what I'm saying is that the fact that some parts of the genome mutate faster than others is something we already know. This isn't necessarily news. The only way I can think that this would be significant is that lab mice are generally thought to be basically genetically identical. They're normally inbred for about 20 generations (most don't survive past 7) to ensure the homozygosity of the mice. Inbred mice like this are valuable because the way they react is consistent and reproducible (traits that are mainstays of science). If they're mutating faster than we expected, it may have an affect on the reliability of the studies done with these mice.
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It would be interesting to know how it allows mutations in this area but not others. (I assume envelope {shell} mutations are needed because the outside surface is how the host immune system identifies it in order to wipe it out. If it wants to hide, then it needs to keep changing its outer coat over generations.)
big variations in sequence lengths and other pol
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It's very similar to the metaphor about the thermos. How does it know to keep cold things cold and hot things hot. It doesn't, it just know, it just does.
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I'd think that it is more likely that packing is more likely to be used to regulate genetic expression. It just happens that as a side effect it is also more protected from modification.
Kind of like having a backup media safe - the purpose of the safe usually isn't to prevent outside theft by professional thieves so much as to prevent casual treatment of media (employees using tapes and leaving them on desks when they are done leaving them susceptible to fir
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The only possibility I can think of is that the region(s) are abnormally variable for a lifeform as complex as a mouse - apples are hardly as sophisticated
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Cellular structure codings are even more invariant than HOX, by the way. If a mutation kills the gonocytes, then it's not a matter of miscarriage like HOX mutations, there's no fertilization out of the starting gate.
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That is, in fact, wrong. Most of the flu strains today are descended from strains fifty or sixty years ago. Usually one of the strains that were emerging in a previous year end up being the dominant strain the next year, buton at least one occasion a couple of years ago, a second, completely unexpected strain turned out to be a codominant strain in many places, making the vaccines much less effective than usual.
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{sarcasm}
Oh! Maybe they blame the scientists for screwing up the mice for that many generations (too many weird chemicals in the lab). After all, scientists aren't examining nature (in which animals don't evolve) in this study. They're examining mice that they trained to evolve! Scientists are making up the so-called evidence right? Yeah, they make freaky mice in a laboratory, but that doesn't mean that everything else evolves does it?
{/sarcasm}
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Misread that.. (Score:1)
That kinda study would be nice, though.
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Maybe organisms with DANGEROUS changes are DEAD??? (Score:1)
OK, forgive me if I'm missing something & this isn't as...
Maybe the organisms with changes in parts of their genome that are not tollerant to change are DEAD....
I would be more surprised if a similar study of stillborn and aborted rats found the same tendency.
Re:Maybe organisms with DANGEROUS changes are DEAD (Score:2, Interesting)
Everyone knows (Score:1, Offtopic)
Everyone knows Tinker Town is the #1 gnome hotspot!
Misinterpretation (Score:4, Informative)