 |
|
University of Chicago study overturns conventional theory in evolution
June 07, 2005New data suggest that the accumulation of genetic changes is not solely determined by natural selection. A study by University of Chicago researchers contradicts conventional theory by showing that the percentage of mutations accepted in evolution is also strongly swayed by the speed at which new mutations arrive at a gene: the faster the speed of new mutations, the greater the percentage of those mutations accepted.
"We've discovered a striking phenomenon that challenges a paradigm of molecular evolution that has been around for several decades," said lead author Bruce Lahn, Ph.D., assistant professor of genetics at the University of Chicago and Howard Hughes Medical Institute investigator. "As such, it may cause a significant shift in the field."
The researchers report their findings in the July 2005, issue of the journal Trends in Genetics, available early online June 7. Other authors are Gerald Wyckoff, Ph.D., previously a postdoctoral fellow in Lahn's lab and now an assistant professor at the University of Missouri-Kansas City, and Christine Malcom and Eric Vallender, both graduate students in Lahn's lab.
For more than three decades, molecular evolutionists have thought that no matter how many genetic mutations show up on a specific gene, whether or not those mutations become fixed in the species is determined primarily by natural selection. The new study shows that the speed at which these new mutations arrive also affects whether the mutations become fixed.
Lahn's team looked at nearly 6,000 genes in their study. For each gene, they compared sequences between two mammalian species. This enabled them to measure the mutation rate of the gene - specifically, the rate of those mutations that do not affect the protein's structure, called synonymous mutation (Ks). These mutations are functionally neutral, which means natural selection is not a factor in whether they are accepted during evolution.
Lahn's team also looked at the mutation rate of nonsynonymous changes (Ka) - the rate of those mutations that do affect protein structure. These mutations are typically subject to natural selection. A nonsynonymous mutation will get accepted into or bounced out of the population based upon how the change alters protein function.
The researchers then studied the Ka/Ks ratio. A low Ka/Ks ratio indicates strong selection; conversely, a high ratio, weak selection. Some genes have a ratio of 0, which means protein changes are not accepted. It is, in a sense, "perfect."
For a pseudogene - a stretch of DNA sequence that resembles a gene but has no function - its Ka/Ks ratio is approximately 1.0, which means that synonymous and nonsynonymous mutations are accepted at the same rate since the gene is functionally irrelevant.
For a gene that is highly functional and important for the organism, its Ka/Ks ratio is typically low. For example, if a gene has a Ka/Ks ratio of 0.1, it means that it's highly selective and is only accepting 10 percent of the nonsynonymous mutations.
Regardless of the rate of new mutations at a particular gene, scientists have always presumed the percentage of nonsynonymous mutations accepted during evolution remains constant.
"This theory has been the workhorse of molecular evolution," Lahn said. "Thousands of scientific papers have been published based directly or indirectly on this notion."
The new data show that if more mutations show up at a gene, that gene tends to accept a higher percentage of those mutations.
"A gene under strong mutational pressure succumbs to that pressure," Lahn said. "For genes that have a high mutation rate, somehow selection appears to become less stringent."
Lahn cannot explain the mechanism of his findings and expects many will question this novel finding. "It's too radical," he said. "People just don't want to believe it, but the data are there."
"Lahn and his associates have found a most striking result, one that is totally unexpected," said geneticist James Crow, professor emeritus of genetics and zoology at the University of Wisconsin-Madison. "If this result is indeed confirmed it would cast doubt on use of this ratio [Ka/Ks] as an indicator of selection."
Sudhir Kumar, an associate professor of molecular evolution at Arizona State University, agreed. "It goes against strict theory, but evolutionary biologists know that nothing's clean cut. There's always distortion because we're looking at longtime history.
"The novelty of this work is that he [Lahn] used a large amount of data," Kumar said. "It's a perfect example of the power of the genome project."
"I hope that further work will provide an explanation of what now is a major puzzle,\\\\\\\
University of Chicago Medical Center
For more than three decades, molecular evolutionists have thought that no matter how many genetic mutations show up on a specific gene, whether or not those mutations become fixed in the species is determined primarily by natural selection. The new study shows that the speed at which these new mutations arrive also affects whether the mutations become fixed.
Lahn's team looked at nearly 6,000 genes in their study. For each gene, they compared sequences between two mammalian species. This enabled them to measure the mutation rate of the gene - specifically, the rate of those mutations that do not affect the protein's structure, called synonymous mutation (Ks). These mutations are functionally neutral, which means natural selection is not a factor in whether they are accepted during evolution.
Lahn's team also looked at the mutation rate of nonsynonymous changes (Ka) - the rate of those mutations that do affect protein structure. These mutations are typically subject to natural selection. A nonsynonymous mutation will get accepted into or bounced out of the population based upon how the change alters protein function.
The researchers then studied the Ka/Ks ratio. A low Ka/Ks ratio indicates strong selection; conversely, a high ratio, weak selection. Some genes have a ratio of 0, which means protein changes are not accepted. It is, in a sense, "perfect."
For a pseudogene - a stretch of DNA sequence that resembles a gene but has no function - its Ka/Ks ratio is approximately 1.0, which means that synonymous and nonsynonymous mutations are accepted at the same rate since the gene is functionally irrelevant.
For a gene that is highly functional and important for the organism, its Ka/Ks ratio is typically low. For example, if a gene has a Ka/Ks ratio of 0.1, it means that it's highly selective and is only accepting 10 percent of the nonsynonymous mutations.
Regardless of the rate of new mutations at a particular gene, scientists have always presumed the percentage of nonsynonymous mutations accepted during evolution remains constant.
"This theory has been the workhorse of molecular evolution," Lahn said. "Thousands of scientific papers have been published based directly or indirectly on this notion."
The new data show that if more mutations show up at a gene, that gene tends to accept a higher percentage of those mutations.
"A gene under strong mutational pressure succumbs to that pressure," Lahn said. "For genes that have a high mutation rate, somehow selection appears to become less stringent."
Lahn cannot explain the mechanism of his findings and expects many will question this novel finding. "It's too radical," he said. "People just don't want to believe it, but the data are there."
"Lahn and his associates have found a most striking result, one that is totally unexpected," said geneticist James Crow, professor emeritus of genetics and zoology at the University of Wisconsin-Madison. "If this result is indeed confirmed it would cast doubt on use of this ratio [Ka/Ks] as an indicator of selection."
Sudhir Kumar, an associate professor of molecular evolution at Arizona State University, agreed. "It goes against strict theory, but evolutionary biologists know that nothing's clean cut. There's always distortion because we're looking at longtime history.
"The novelty of this work is that he [Lahn] used a large amount of data," Kumar said. "It's a perfect example of the power of the genome project."
"I hope that further work will provide an explanation of what now is a major puzzle,\\\\\\\
University of Chicago Medical Center
Gene Mutations Current Events and Gene Mutations News RSSSchizophrenia gene's role may be broader, more potent, than thought
UCSF scientists studying nerve cells in fruit flies have uncovered a new function for a gene whose human equivalent may play a critical role in schizophrenia.
Time in a bottle: Scientists watch evolution unfold
A 21-year Michigan State University experiment that distills the essence of evolution in laboratory flasks not only demonstrates natural selection at work, but could lead to biotechnology and medical research advances, researchers said.
Stanford scientist's new findings of autism-associated synapse alterations lead to coveted NIH grant
A Stanford University School of Medicine researcher has pinpointed the mechanism by which a gene associated with both autism and schizophrenia influences behavior in mice. And just recently, he received a $1.65 million government grant to expand his efforts to include many more such genes.
Gene mingling increases sudden death risk
A multi-national research team has discovered that two genetic factors converge to increase the risk of sudden cardiac death.
Chinese and American paleontologists discover a new Mesozoic mammal
An international team of paleontologists has discovered a new species of mammal that lived 123 million years ago in what is now the Liaoning Province in northeastern China.
Amyotrophic lateral sclerosis may involve a form of sudden, rapid aging of the immune system
Premature aging of the immune system appears to play a role in the development of amyotrophic lateral sclerosis (ALS), or Lou Gehrig's disease, according to research scientists from the Maxine Dunitz Neurosurgical Institute at Cedars-Sinai Medical Center, the Weizmann Institute of Science in Israel, and Sheba Medical Center in Israel.
Evolution coup: Study reveals how plants protect their genes
Unlike animals and humans, plants can't run and hide when exposed to stressful environmental conditions. So how do plants survive?
New research strategy for understanding drug resistance in leukemia
UCSF researchers have developed a new approach to identify specific genes that influence how cancer cells respond to drugs and how they become resistant. This strategy, which involves producing diverse genetic mutations that result in leukemia and associating specific mutations with treatment outcomes, will enable researchers to better understand how drug resistance occurs in leukemia and other cancers, and has important long-term implications for the development of more effective therapies.
Breast cancer: Risk increases for smokers and overweight women
A recent study published in the Journal of Cancer Epidemiology has reinforced the correlation between being overweight, smoking and breast cancer.
Computational Process Zeroes in on Top Genetic Cancer Suspects
Johns Hopkins engineers have devised innovative computer software that can sift through hundreds of genetic mutations and highlight the DNA changes that are most likely to promote cancer.
More Gene Mutations Current Events and Gene Mutations News Articles
 |
Gene: Gene. History of genetics, Mendelian inheritance, Gene expression, Genetic code, Mutation, Gene targeting, The Selfish Gene, Copy number variation, ... Gene- centered view of evolution by Frederic P. Miller (Editor), Agnes F. Vandome (Editor), John McBrewster (Editor) Gene. History of genetics, Mendelian inheritance, Gene expression, Genetic code, Mutation, Gene targeting, The Selfish Gene, Copy number variation, DNA, Epigenetics, Gene- centered view of evolution, Gene therapy, Genetic algorithm, Genetics, Genome, Genomics, List of human genes, Meme, Pseudogene, Predictive medicine |
 |
ABC News Nightline Confronting a Genetic Legacy Imagine you were told that you carry a gene that makes it all but certain you will one day get breast cancer, ovarian cancer or both. What would you do? Jessica Queller, a 35-year-old writer for the hit series "Gilmore Girls," has had to answer that question. In 2004, she found out that she carries the BRCA1 gene mutation, or, the breast cancer gene. According to one study, possessing that gene means she has an 85 percent chance of developing breast cancer before the age of 70 and a 50 percent chance of developing it before the age of 50. Queller took the test because her mother had recently died of ovarian cancer, and several years earlier had fought and beaten breast cancer. Queller now knows what her mother never did, and now she is left in a place where modern science has told her... |
|
Mutation linked to some cases of Parkinson's: identifying gene raises ethical questions about its use in testing, given the lack of preventive therapy.(Neuropsychiatric ... An article from: Clinical Psychiatry News by Christine Kilgore (Author) This digital document is an article from Clinical Psychiatry News, published by International Medical News Group on April 1, 2005. The length of the article is 933 words. The page length shown above is based on a typical 300-word page. The article is delivered in HTML format and is available in your Amazon.com Digital Locker immediately after purchase. You can view it with any web browser. Citation Details Title: Mutation linked to some cases of Parkinson's: identifying gene raises ethical questions about its use in testing, given the lack of preventive therapy.(Neuropsychiatric Medicine) Author: Christine Kilgore Publication: Clinical Psychiatry News (Magazine/Journal) Date: April 1, 2005 Publisher: International Medical News Group Volume: 33 Issue: 4 Page:... | |
|
MRI best for carriers of BRCA gene mutations: study shows MRI detects more breast cancers in this population than do ultrasound or mammography.(Women's ... An article from: Family Practice News by Betsy Bates (Author) This digital document is an article from Family Practice News, published by International Medical News Group on December 1, 2004. The length of the article is 979 words. The page length shown above is based on a typical 300-word page. The article is delivered in HTML format and is available in your Amazon.com Digital Locker immediately after purchase. You can view it with any web browser. Citation Details Title: MRI best for carriers of BRCA gene mutations: study shows MRI detects more breast cancers in this population than do ultrasound or mammography.(Women's Health)(Magnetic resonance imaging) Author: Betsy Bates Publication: Family Practice News (Magazine/Journal) Date: December 1, 2004 Publisher: International Medical News Group Volume: 34 Issue: 23 Page:... | |
![Mouse lymphoma thymidine kinase gene mutation assay: Meeting of the International Workshop on Genotoxicity Testing, San Francisco, 2005, recommendations ... Toxicology and Environmental Mutagenesis]](http://ecx.images-amazon.com/images/I/51VRJGWFK9L._SL160_.jpg) |
Mouse lymphoma thymidine kinase gene mutation assay: Meeting of the International Workshop on Genotoxicity Testing, San Francisco, 2005, recommendations ... Toxicology and Environmental Mutagenesis] by M.M. Moore (Author), M. Honma (Author), J. Clements (Author), G. Bolcsfoldi (Author) This digital document is a journal article from Mut.Res.-Genetic Toxicology and Environmental Mutagenesis, published by Elsevier in 2007. The article is delivered in HTML format and is available in your Amazon.com Media Library immediately after purchase. You can view it with any web browser. Description: The Mouse Lymphoma Assay (MLA) Workgroup of the International Workshop on Genotoxicity Testing (IWGT), comprised of experts from Japan, Europe and the United States, met on September 9, 2005, in San Francisco, CA, USA. This meeting of the MLA Workgroup was devoted to reaching a consensus on issues involved with 24-h treatment. Recommendations were made concerning the acceptable values for the negative/solvent control (mutant frequency, cloning efficiency and suspension growth)... |
|
Frequency of the 35delG mutation in the GJB2 gene in samples of European, Asian, and African Brazilians.: An article from: Human Biology by C.A. Oliveira (Author), F. Alexandrino (Author), K. Abe-Sandes (Author), W.A. Silva (Author), A.T. Maciel-Guerra (Author), L.A. Magna (Author), E.L. Sartorato (Author) This digital document is an article from Human Biology, published by Wayne State University Press on April 1, 2004. The length of the article is 1423 words. The page length shown above is based on a typical 300-word page. The article is delivered in HTML format and is available in your Amazon.com Digital Locker immediately after purchase. You can view it with any web browser. From the author: KEY WORDS: GJB2, BRAZILIAN POPULATION, CONGENITAL DEAFNESS Citation Details Title: Frequency of the 35delG mutation in the GJB2 gene in samples of European, Asian, and African Brazilians. Author: C.A. Oliveira Publication: Human Biology (Refereed) Date: April 1, 2004 Publisher: Wayne State University Press Volume: 76 Issue: 2 Page: 313(4) Distributed by... | |
![American Cancer Society Film: Time is Life (1949) [DVD]](http://ecx.images-amazon.com/images/I/416uIWyVduL._SL160_.jpg) |
American Cancer Society Film: Time is Life (1949) [DVD] Time is Life highlights the importance of time in combating the second highest cause of death in the world, cancer. The film also underscores the efforts of the American Cancer Society towards the alleviation, if not elimination, of cancer in the American society. The film starts with Mary Bronson being stressed out with the possibility of having a cancer. Cancer is not given proper attention by the public so it causes insurmountable effects on people in the society. Cancer chooses no one. In addition, the film gives conveying figures on cancer fatalities in the United States saying that one in every eight American has cancer. The film has also mentioned that cancer has killed more Americans than the slaughter at the Pearl Harbor and Tokyo Bay during World War Two. The film also dispels... |
|
Screening of APOB gene mutations in subjects with clinical diagnosis of familial hypercholesterolemia.: An article from: Human Biology by Erardo Merino-Ibarra (Author), Sergio Castillo (Author), Pilar Mozas (Author), Ana Cenarro (Author), Esperanza Martorell (Author), Jose Luis Diaz (Author), Manuel Suarez-Tembra (Author), Rodrigo Alonso (Author), Fernando Civeira (Author), Pedro Mata (Author), Miguel Pocovi (Author) This digital document is an article from Human Biology, published by Thomson Gale on October 1, 2005. The length of the article is 4221 words. The page length shown above is based on a typical 300-word page. The article is delivered in HTML format and is available in your Amazon.com Digital Locker immediately after purchase. You can view it with any web browser. From the author: KEY WORDS: FAMILIAL DEFECTIVE APOB, AUTOSOMAL DOMINANT MONOGENIC HYPERCHOLESTEROLEMIA (ADMH), HYPERCHOLESTEROLEMIA, APOB, LDLR, R3500Q MUTATION, T3552T MUTATION, SSCP (SINGLE-STRAND CONFORMATION POLYMORPHISM) ANALYSIS, SPAIN. Citation Details Title: Screening of APOB gene mutations in subjects with clinical diagnosis of familial hypercholesterolemia. Author: Erardo... | |
|
Key estrogen receptor gene mutation discovered. (Clinical Rounds: May be exploitable as a prognostic factor).(Brief Article): An article from: Internal Medicine News by Bruce Jancin (Author) This digital document is an article from Internal Medicine News, published by International Medical News Group on April 1, 2002. The length of the article is 2913 words. The page length shown above is based on a typical 300-word page. The article is delivered in HTML format and is available in your Amazon.com Digital Locker immediately after purchase. You can view it with any web browser. Citation Details Title: Key estrogen receptor gene mutation discovered. (Clinical Rounds: May be exploitable as a prognostic factor).(Brief Article) Author: Bruce Jancin Publication: Internal Medicine News (Magazine/Journal) Date: April 1, 2002 Publisher: International Medical News Group Volume: 35 Issue: 7 Page: 24(1) Article Type: Brief Article Distributed by... | |
|
657del5 mutation of the Nijmegen breakage syndrome gene (NBS1) in the Turkish population.(Author Abstract): An article from: Human Biology by Mustafa Tekin (Author), Duygu Akcayoz (Author), Canan Ucar (Author), Huseyin Gulen (Author), Nejat Akar (Author) This digital document is an article from Human Biology, published by Thomson Gale on June 1, 2005. The length of the article is 1366 words. The page length shown above is based on a typical 300-word page. The article is delivered in HTML format and is available in your Amazon.com Digital Locker immediately after purchase. You can view it with any web browser. From the author: KEY WORDS: FOUNDER EFFECT, NIJMEGEN BREAKAGE SYNDROME, NBS1, SLAVS, TURKS. Citation Details Title: 657del5 mutation of the Nijmegen breakage syndrome gene (NBS1) in the Turkish population.(Author Abstract) Author: Mustafa Tekin Publication: Human Biology (Magazine/Journal) Date: June 1, 2005 Publisher: Thomson Gale Volume: 77 Issue: 3 Page: 393(5) Article Type: Author... |
| © 2009 BrightSurf.com |