SOME GENETIC RESEARCH IS BEST DONE CLOSE TO THE EVOLUTIONARY HOME

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SOME GENETIC RESEARCH IS BEST DONE CLOSE TO THE EVOLUTIONARY HOME
03 July 2006 - DOE/Lawrence Berkeley National Lab

Some aspects of evolution are like the real estate business in that it's all about location, location, location! Researchers with the U.S. Department of Energy's Lawrence Berkeley National Laboratory and the DOE Joint Genome Institute have shown that when it comes to comparing evolutionarily conserved DNA sequences that regulate the expression of genes, more closely related species are best.

"While one can compare distant vertebrates to humans and identify sequences that are highly evolutionarily conserved, such elements are few and far between," said Len Pennacchio, a geneticist with Berkeley Lab's Genomics Division and the head of JGI's genome analysis program. "In contrast, by comparing species that are more closely related, such as other mammals, we can find much more DNA sequence alignment."

Pennacchio and Shyam Prabhakar are the principal authors of a paper that appears in the June issue of the publication Genome Research, which presents the results of a comparative genomics study that quantified the advantages of staying close to the evolutionary home. Other co-authors of the paper were Francis Poulin, Malak Shoukry, Veena Afzal, Edward Rubin and Olivier Couronne.

When Mother Nature develops something that works, she tends to stick with it. Hence sequences of DNA that serve as protein-coding genes or enhancers that regulate the expression of those genes have been conserved through thousands of years of evolution. Gene hunters have capitalized on this tendency by comparing the DNA of different species to identify genes and determine their functions. For example, the genome of the Fugu fish contains essentially the same genes as the human genome but carries them in approximately 400 million bases as compared to the three billion bases that make up human DNA.

Cross-species DNA sequence comparisons have also been used to identify the enhancers that regulate genes, meaning they control whether a gene is switched on or off, but until now, the relative merits of comparing species as diverse as humans and fish were not known.

"To address this problem, we identified evolutionarily conserved non-coding regions in primate, mammalian and more distant species using a uniform approach that facilitates an unbiased assessment of the impact of evolutionary distance on predictive power," said Pennacchio. "We benchmarked computational predictions against previously identified regulatory elements at diverse genomic loci, and also tested numerous extremely conserved sequences in humans and rodents for enhancer activity."

The computational algorithm, which is used to provide a uniform evaluation of the benefits and limitations of DNA sequence comparisons between close versus distant species, was developed by Prabhakar. He dubbed this program "Gumby," after a mathematical concept called the Gumbel distribution. Prabhakar's Gumby program has now been incorporated into VISTA, the comprehensive suite of programs and databases for comparative analysis of genomic sequences that was developed and is maintained at Berkeley Lab.

Using the Gumby program, Prabhakar, Pennacchio and their colleagues were able to identify human regulatory DNA sequences with a sensitivity that ranged from 53 to 80 percent, and a true-positive rate that ran as high as 67 percent based on comparisons with primates and other eutherian (placental) mammals. By contrast, comparisons with more distant species, including marsupial, avian, amphibian and fish, failed to identify most of the empirically defined functional non-coding DNA sequences.

Said Prabhakar, "Our results highlight the practical utility of close sequence comparisons, and the loss of sensitivity entailed by more distant comparisons. The intuitive relationship we derived between ancient and recent non-coding sequence conservation from whole-genome comparative analysis explains most of the observations from empirical benchmarking."

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About: DOE/Lawrence Berkeley National Lab
Lawrence Berkeley National Laboratory (Berkeley Lab) has been a leader in science and engineering research for more than 70 years. Located on a 200 acre site in the hills above the Berkeley campus of the University of California, overlooking the San Francisco Bay, Berkeley Lab is a US Department of Energy (DOE) National Laboratory managed by the University of California. It has an annual budget of nearly $480 million (FY2002) and employs a staff of about 3,900, including more than a thousand students.

Berkeley Lab conducts unclassified research across a wide range of scientific disciplines with key efforts in fundamental studies of the universe; quantitative biology; nanoscience; new energy systems and environmental solutions; and the use of integrated computing as a tool for discovery. It is organized into 17 scientific divisions and hosts four DOE national user facilities. Details on Berkeley Lab’s divisions and user facilities can be viewed here.

The Lab was founded in 1931 by Ernest Orlando Lawrence, winner of the 1939 Nobel Prize in physics for his invention of the cyclotron, a circular particle accelerator that opened the door to high-energy physics. It was Lawrence’s belief that scientific research is best done through teams of individuals with different fields of expertise, working together. His teamwork concept is a Berkeley Lab legacy that has yielded rich dividends in basic knowledge and applied technology, and a profusion of awards, including nine Nobel Prizes -- five in physics and four in chemistry.

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