Now, scientists at The Wistar Institute have shown that MYC activates a gene called MTA1, which has been demonstrated by other researchers to regulate metastasis in a variety of cancers. While researchers have been exploring the possibility of blocking MTA1 to prevent metastasis, it was not previously known how MTA1 becomes activated in the first place. The study adds to the emerging picture of MYC's role in cancer development and progression and identifies the pathway linking MYC and MTA1 as an area for further exploration into the genetics of metastasis. The study appears in Proceedings of the National Academy of Sciences and is available in the journal's online "Early Edition."
"We and others have been working to understand what genes MYC turns on to cause malignant transformation," says Wistar associate professor Steven B. McMahon, Ph.D., senior author of the study. "Understanding metastasis is critical because patients rarely die of primary tumors--metastasis usually causes cancer deaths. Now, we have linked the well-known oncogene MYC to this target gene, MTA1, a key regulator of metastasis. Most importantly, if we block MYC's ability to turn on MTA1, we block tumor formation. This is critical because it identifies a point in the metastasis pathway that can be targeted therapeutically."
Like the MYC cancer gene, MTA1 has been shown to play a role in a wide range of cancers, including breast and lun
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Contact: Marion Wyce
wyce@wistar.org
215-898-3943
The Wistar Institute
12-Sep-2005