In the new era of personalized medicine, physicians hope to provide earlier diagnoses and improve therapy byevaluating patients' genetic blueprints. But, as a new bioinformatics study emphasizes, the first step must be tocorrectly decipher the deluge of information locked in our DNA and determine its impact on human health.
In the September issue of Genome Research, Dr. Sudhir Kumar led a team of researchers at the BiodesignInstitute at Arizona State University in examining DNA mutations from both healthy and diseased patients.Their work evaluates the reliability of computer models aimed at predicting the eventual effect of suchmutations.
Along with Kumar, director of the Biodesign Institute's Center for Evolutionary Functional Genomics, othersinvolved with the study were co-authors Michael P. Suleski, Glenn J. Markov, Simon Lawrence, AntonioMarco and Alan J. Filipski.
Kumar's team focused on single DNA mutations—changes to a person's genome that can sometimes make thedifference between robust health and debilitating illness. The current study focused on one specific type ofDNA mutation—a single change at a given location along the length of DNA—that alters the resulting protein.These protein changes are the source of much of our individuality, coding for differences such as eye and haircolor. Scientists have discovered that each person's genome contains thousands of such protein changes. Othersingle mutations, however, are linked with severe illnesses like cystic fibrosis.
While experimentation on the enormous number of mutations across human populations is impractical due tovolume and cost, Mother Nature, as Kumar points out, has already done an experiment for us, presentingscientists with a set of benign mutations for each protein. The branch of science known as comparativegenomics takes advantage of the genetic information collected from the diversity of life on Earth.
We now know that humans display a striking degree of genetic similarity with many other species, particularlynon-human primates like chimpanzees, gibbons, gorillas and orangutans, with whom we share over 98 percentof our genes. "Comparative genomics provides the first clues as to what a mutation might mean," says Kumar."This is an area that is going to become center stage in personal genomics and medicine."
Techniques in this rapidly expanding field make use of existing Web databanks such as GenBank, whichcontains more than 100 billion DNA and protein sequence elements collected from all walks of life. "Thesedatabases already contain the outcomes of nature's experiment, which we can harness by using bioinformatics,"says Kumar.
DNA medicine typically uses a suite of computer tools to assess whether a newly discovered protein change ispotentially disease-causing or benign. Kumar's study tested the reliability of two of the most widely-used tests,known as SIFT and PolyPhen, by examining over 20,000 mutations from both diagnosed patients and healthyindividuals. The results demonstrate that these tests make false predictions of risk up to 40 percent of the time, arate of reliability that renders them impractical for clinical use.
The objective of the study was to identify where SIFT and PolyPhen tend to fail and where their predictionsappear to be more reliable. To accomplish this, Kumar's group examined the proteins in 44 species, from frogsto fish, chimps and gorillas. His group discovered that benign mutations tend to occur in regions of the genomethat allow variation over evolutionary time across species. In these regions, it is easier to make accuratepredictions of benign mutations.
In contrast, DNA information essential for life is persistent from species to species. Many DNA positionspermit no change over evolutionary time in order to preserve proper function—mutations here would likely bedamaging. Reinforcement of this theory was found in the subset of mutations discovered in disease-associatedgenes. Such mutations are clustered in positions of the genome that are conserved over evolutionary time or inmutant protein sequences that are rarely seen. Amazingly, less than 10 percent of known single gene diseasemutations are ever found in other species.
As Kumar notes, evolution has provided researchers with a storehouse of genetic mutations, many of which willprove benign for human health. "Suppose you had a mutation at a certain position," he explains, "and your doghas the same change as you have. It's most likely that that change is not harmful." By the same token, if noother species contains the mutation found in one's genome, it calls for further investigation.
Kumar stresses that it will take a combination of additional DNA sequencing data and improved understandingof protein function to refine the power of computer analyses. In the meantime, his bioinformatics evaluations ofcurrent computer tools suggest where such tests may be appropriately used for diagnosis with higher confidenceand where their results are more likely to be unreliable.
With the costs of rapid DNA sequencing plummeting, individual genetic profiling is already becoming popular,offering every patient access to an enormous treasure trove of medically-relevant information. According toKumar, the ultimate challenge will be sorting out what all this genetic information implies for each individual'sprognosis. Only then will the promise of personalized medicine be fully realized.
Source: Arizona State University