These few examples were found primarily by luck, but now with the availability of multiple mammalian genome sequences, researchers can systematically search for human genes that show signs of being adaptively lost at some point in our history. David Haussler's group at UC Santa Cruz, in a recent paper, looked for the genes we lost as we developed into our modern-day human species. What they found could help us better understand our evolutionary history, and possibly the human diseases that are the side-effects of that history.
It's not hard to find genes that have been lost in the human genome - our genomes are littered with pseudogenes, genes which harbor inactivating mutations making them unable to produce a functional protein. But most of these damaged genes have functional copies elsewhere in the genome. Genes are frequently duplicated in the random shuffling that goes on in our chromosomes, and often the duplicate copy will be destroyed by mutations while the good copy continues to perform its original function. Another frequent phenomenon is the production of processed pseudogenes - these are genes that were produced when RNA was transcribed back into DNA and integrated into the genome. The result is a gene that looks just like a highly processed RNA molecule, often surrounded by the classic genetic residue that is left behind when a piece of DNA is integrated back into the genome.
Looking for lost genes
Haussler's group was not interested in these two relatively mundane classes of pseudogenes; they were searching for genes that are clearly functional in other mammals, and which have not been duplicated or reverse transcribed from RNA. In other words, the genes they were looking for would have no other functional copies hanging around somewhere else in the genome. Genes in this category are likely to be candidates for adaptive losses - genes whose function has been completely eliminated from the human genome, which may have provided some benefit to the original ancestor in which the gene was lost.
These researchers performed their search by comparing functional genes in the mouse genome with genes in the human and dog genomes. Mice are more closely related to humans than dogs are; a gene that is present and functional in mice and dogs, but destroyed by mutation in humans has therefore been present in mammals for a very, very long time, but was recently lost in the human lineage.
You can see how this works in the figure below (which I have marked up slightly from the original version in the paper). The mouse and human versions of our hypothetical gene line up nicely, but there is an inactivating mutation in the human version. In the dog version (not shown), that mutation is absent.
What they found
After completing their genome scan, and applying various quality control filters, Haussler's group came up with 72 candidate lost genes. They found some well-known lost genes, such as GULO, an enzyme necessary for making vitamin C that was been destroyed in primates, but is still functional in most other mammals. (If we still had a functional copy of this gene, we wouldn't get scurvy.)
Thee researchers found new lost genes as well, most of which have poorly characterized functions. One gene, named ACYL3 (NM_177028 in the mouse genome, for those of you who want to check out GenBank), contains a very highly conserved enzyme structure, called an acyltransferase domain (see more here). This particular acyltransferase domain is very ancient - it is found in bacteria, archaea, plants, fungi, and animals. Many species have multiple copies of this domain (the fruitfly has over 30), but mammals have only a few copies, and humans have absolutely no functional copies. We know almost nothing about this gene: it produces a membrane protein, it is expressed in the mouse pituitary gland, and it is necessary for normal embryo development in worms and flies. Why was it lost in humans, and was that loss beneficial? We don't know yet. Do we get some diseases that mice don't get, because we lack this gene? It would be fascinating to find out.
Although we know little about ACYL3, Haussler's group was able to pinpoint the timeframe of the loss. This gene was destroyed by a nonsense mutation, a change from TGG (coding for the amino acid tryptophan) to TGA, which means stop - the protein is truncated right in the middle of a highly conserved region. This TGG to TGA change is found only in chimps and humans, not gorillas, orangutans, or any other mammals checked. The mutation therefore happened after the chimp-human lineage split off from the other great apes. Gorillas and orangutans have a functional ACYL3 gene; humans and chimps don't.
Other lost genes found by these researchers included genes lost in only chimps, gorillas and humans, genes lost in all great apes, and genes lost in primates. Each of these losses is an example of an ancient gene that was functional for hundreds of millions of years, but then lost very recently in the lineage that led to primates, and ultimately humans. Without detailed functional studies in multiple species, it is hard to know which genes were lost adaptively, providing an immediate benefit sustained by natural selection, and which were lost simply because they were no longer necessary in a particular environment (such as the vitamin C biosynthesis enzyme). But with this list of genes in hand, we know where to start. It would be fascinating to figure if any of these lost genes are linked to human diseases (like GULO and scurvy), since the lost function could provide an important clue regarding the mechanism of the disease.
It's worth noting the implications of studies like this for the creation-evolution debate. Creationists, including most of the major advocates for its latest form, Intelligent Design, have frequently expressed their disbelief in human evolution and the common ancestry of today's species. In the case of ACYL3, the only plausible explanation for the pattern of mutation that Haussler's group found is that humans and chimps shared a common ancestor. If humans and chimps had been created de novo as separate species, it would an be extremely unlikely coincidence for these identical mutations to occur by chance individually in each species. And when you factor in the distribution of dozens, hundreds, thousands of such mutations, all occurring in a similar pattern, it becomes not just unlikely but essentially impossible that such patterns of mutation would have arisen by chance in each separately created species. One could suggest that a designer just decided to arrange things this way, but that argument falls in the same class as the claim that God just made the universe and the earth appear old, after creating it all 10,000 years ago. There is simply no rationale based on evidence to question the fact of common descent, and those who continue to resist this fact can only do so for religious or psychological reasons.
Figures from the original paper were annotated, cropped and posted under the PLoS Open Access License.
4 comments:
I should expand on the suggestion that these lost genes could shed light on the mechanism underlying some human diseases. How would we know whether one of these dead genes is connected to a disease? Take the case of ACYL3 for example - since this gene is long dead in humans, you won't find humans with disease-conferring mutants in ACYL3, which is how you typically find a gene linked to a disease.
What you do is study the function of recently lost genes in mice, or say, Rhesus monkeys (who do have a functional ACYL3, for example). When you've found the biological processes that such genes are involved in, the next step is to see which diseases are connected with that particular biological process in humans, and to check whether those diseases are non-existent or different in mice. This is not easy work, but it could generate some interesting and possibly worthwhile hypotheses.
In sum, this is an argument for studying certain genes that are not present in humans, something which hasn't necessarily been a priority in mouse research.
The paper is a good example how to sell results from genomics: Come up with an interesting but relatively solvable question, throw in a team of excellent programmers, then pick out one or two of the most outstanding results (there will always be some) and do some reading on the genes. Discuss the results.
Go on to the next question: ultraconserved fragments, conserved introns, novel exons, the fastest evolving regions, the slowest evolving regions.... etc. Haussler's team is following this strategy very often, like many groups in genomics.
This is not a negative comment, I definitely like the papers from the UCSC bioinformatics group. It's kind of different from many researchers that completely stick to their question for many years instead of picking out outstanding examples from a whole-genome analysis.
You're absolutely right - many groups do computational genome analysis, but never get to any follow up. You get lists of genes or other features like ultraconserved elements, and then people just move on to the next big analysis.
Hypothesis testing with real experiments is good. People should do more of it.
Thanks Mike, you raise many relevant issues and your discourse is well conceived and clearly expressed.
Perhaps you have already moved on but would you consider examining the possibility that a disabled gene confers benefits as well as liabilities? Take the faulty GULO gene, for example, both people and chimpanzees have access to abundant fruit which contains the scurvy antidote, "vitamin C". The advantage is, more glucose for energy and fat production. If faulty GULO increases blood glucose available for these other functions, we and the monkeys have an advantage over others not blessed with this defect? Since fruit also contains sugars which further augment glucose resources we score big! Babies in maternity wards choose supplementary sugar water over milk in the majority of cases. Is this why are we and our simian cousins are programmed to seek sweet? If a dietary proclivity leads to a surfeit of fat and obesity is a risk factor in heart disease, can it be said that the damaged GULO gene is the genetic cause of heart disease? If so, that's a distinct disadvantage to someone who wants to live over 40 without medical interventions.
I would like to hear more of your views on this subject and hope you will comment further. Perhaps you are familiar with the work of WW Wells with guinea pigs at the University of Michigan or Peter Vogeli's work with scorbutic Danish porkers. Both bear on the GULO subject matter. Warm regards, DanD.
Ref: http://lib.bioinfo.pl/auth:V%C3%B6geli,P
P.S. My field is Sociology and we are notorious for collecting endless data and seldom getting around to analyzing or collating it. Of course, "we" does not mean "I". DD
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