News Release

Hundreds of cancer possibilities arise from common skin mole mutation

Peer-Reviewed Publication

Houston Methodist

Skin Nevus

image: The mutation BrafV600E is found in 70 percent or more of benign birthmarks and moles in humans. Scientists believe the Braf mutation alone isn't enough to cause cancer. A variety of subsequent mutations identified in the present study, however, make melanomas possible. view more 

Credit: Houston Methodist

HOUSTON -- ( April 23, 2015 ) -- A Houston Methodist-led team of international scientists has identified hundreds of possible new genes in mice that could transform benign skin growths into deadly melanomas.

An initial mutation, called BrafV600E, is found in 70 percent or more of benign birthmarks and moles in humans, and has long been believed to precede the development of melanomas, even though the Braf mutation alone does not seem to be enough to cause cancer. What skin cancer researchers have not had -- until the present report in Nature Genetics -- is a list of genes or genetic pathways that, once altered, work with the Braf mutation to cause cancer.

"We want to know what exactly must happen after someone acquires this mutation in Braf that causes something even worse to happen," said Houston Methodist Research Institute cancer geneticist Michael Mann, Ph.D., the Nature Genetics report's lead author. "We want to understand how this Braf mutation makes people vulnerable... susceptible to melanoma, so that we can help identify new targets for slowing or stopping growth."

The scientists used a genetic tool, a transposon called "sleeping beauty" that was developed by Houston Methodist cancer geneticists Nancy Jenkins, Ph.D., and Neal Copeland, Ph.D., and an animal model developed by UC San Francisco cancer geneticist Martin McMahon, Ph.D., to identify the candidate cancer genes, or CCGs, that unleash BrafV600E's terrible potential.

"By using Sleeping Beauty strategically, our group was able to identify an incredible number of genes that may cause nevi -- moles and other skin marks -- to become cancerous," Mann said. "As we expected, we haven't just identified single genes that respond to the Braf mutation, but whole pathways that appear to contribute to cancer development. This is important, because if you look at it tumor by tumor, the same pathways may appear to be engaged, but not because of changes to the same genes. If you looked only at singular genes, you could miss what is really going on, biologically."

By letting Sleeping Beauty loose in the model's genome and looking for meaningful outcomes, the scientists were able to identify 1,232 altered CCGs that, with BrafV600E, led to melanomas.

A comparison of human genes equivalent to those the scientists identified in mice showed that more than 500 human genes, sampled from melanoma patients, were "enriched" for mutations and that these mutations appeared to be related to patient survival. A genetic survey of human melanoma patients whose skin biopsies already contain BrafV600E and other relevant mutations could be helpful to oncologists in predicting patient outcomes.

Last, the researchers found that one human gene, CEP350, appears to be required for tumor suppression. CEP350 had not previously been named a melanoma tumor suppressor gene. CEP350 encodes a protein believed to be crucial for cell division.

Cancers of the skin are the most common form of cancer. In the U.S., the American Cancer Society estimates nearly 10,000 will die from metastatic melanomas by year's end. Globally, the World Heath Organization estimates one person dies from melanoma every 50 seconds.

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Also contributing to the Nature Genetics manuscript were Michael A. Black (University of Otago, N.Z.), Devin J. Jones, Justin Y. Newberg, Neal Copeland, and Nancy Jenkins (Houston Methodist), Jerrold M. Ward (Global VetPathology, Md.) Christopher Chin Kuan Yew (National Heart Research Institute Singapore), Adam J. Dupuy (University of Iowa Carver College of Medicine), Alistair G. Rust (Institute of Cancer Research, London, U.K.), Marcus W. Bosenberg (Yale School of Medicine), Martin McMahon (UC San Francisco), and Cristin G. Print (University of Auckland, N.Z.). Research was funded by the National Cancer Institute, the Agency for Science, Technology, and Research, Singapore, the Cancer Prevention Research Institute of Texas, the Health Research Council of New Zealand, the University of Auckland, the New Zealand Maurice Wilkins Centre, and the Melanoma Research Alliance.

To speak with Dr. Michael Mann, please contact David Bricker, Houston Methodist, at 832-667-5811 or dmbricker@houstonmethodist.org.


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