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Genome update defines landscape of breast and colon cancers
Their report, published online in the October 11 issue of Science Express, indicates that while little is known about these less-usually mutated genes, they can be grouped into clusters as per their pathways.
There are gene mountains represented by those that are frequently altered and have been the focus of cancer research for years, in part because they were the only genes known to contribute to cancer, says Bert Vogelstein, M.D., an investigator at the Howard Hughes Medical Institute and co-director of the Ludwig Center at Johns Hopkins. Now, we can see the whole picture, and it is clear that lower peaks or gene hills are the predominant feature.
In a systematic search of 18,191 genes representing more than 90 percent of the protein-coding genes in the human genome -- about 5,000 more than in the first screen -- the Johns Hopkins researchers observed that most cancer-causing gene mutations are quite diverse and can vary from person to person. They observed that an average 77 genes are mutated in an individual colon cancer and 81 in breast cancer. Of these, about 15 are likely to contribute to a cancers key characteristics, and most of these genes may be different for each patient.
Fifteen years ago, we said the p53 gene was the most usually mutated gene in cancer. Its amazing that this is still true, says Kenneth W. Kinzler, Ph.D., professor of oncology at Hopkins Kimmel Cancer Center.
With no more higher-frequency mutations on the horizon, the researchers say that personalized medicines may now focus on the more complicated pathways that link these less-usually mutated genes.
As an example, the Hopkins team charted the path of nine genes less frequently mutated in breast or colon cancers. Each of the genes protein products interacted with an average of 25 other proteins, encoded by separate genes also found to be mutated in the cancers. It suggests that these genes converge in similar pathways. The hard part used to be finding these mutant genes, now the challenge will be to link them to specific pathways and understand their function, says Victor Velculescu, M.D., Ph.D., associate professor of oncology at the Johns Hopkins Kimmel Cancer Center.
The researchers say that directing therapies at common pathways that are linked by both prevalent and rare gene mutations is a better approach than aiming therapys at specific genes. They also note that personalized cancer genomics paves the way for tailored therapies and diagnostics focusing on the alterations identified in a particular patients cancer. A number of of the mutations identified by researchers could be important in developing individualized cancer vaccines and monitoring patients for early recurrence of their disease.
For the study, the researchers screened the same set of tissue samples that were used for their first genome draft - 11 each of breast and colorectal cancers, removed from patients after surgery. Then, they reviewed all mutated genes in a second group of 24 samples from each cancer, and a subset of the most promising mutations were studied in a further 96 colorectal cancers. They compared the genetic sequence of these tumors with that of normal tissue samples from the same patients using computer software that matches up gene codes in cancer and normal cells.
Within each cell, chemicals called nucleotides pair up to form the rungs of a DNA ladder that carry genetic instructions guiding everything from cell-to-cell contact to eye color. Changes in the nucleotide arrangement can create errors in the proteins made from the DNA. Buildup of damaged proteins can turn a normal cell into a malignant one.
Laura Wood, a postdoctoral fellow at Hopkins Kimmel Cancer Center says that these results can help to direct the global race to map additional cancer genomes. For other cancers, she says researchers should expect to find a similar genetic landscape - few mountains surrounded by a number of hills.
Posted by: Jessica Source