2 min readSecond Mutation in BRAF-mutated Metastatic Melanoma Does Not Contribute to Drug Resistance
Los Angeles, CA – UCLA scientists studying the ways in which skin cancer becomes resistant to drug treatment have discovered that a second mutation found in the tumours of patients with BRAF-mutated metastatic melanoma does not contribute to resistance to BRAF inhibitor drugs, a finding that runs counter to what they expected.
The study by researchers at UCLA’s Jonsson Comprehensive Cancer Center found that patients with mutations in both the MEK1 and BRAF genes respond as well to the inhibitors as patients with the BRAF mutation alone.
Another surprising finding is that the MEK1 and BRAF mutations exist together in these patients, despite the fact that they drive the same cell signalling pathway. That discovery also bucks conventional wisdom, said the study’s senior author, Dr. Roger Lo, an assistant professor of dermatology and molecular and medical pharmacology at UCLA and a Jonsson Cancer Center scientist.
“This study is a good example of why scientists should not always rely on what we expect to find,” Lo said. “We expected that this second mutation was involved in drug resistance, and it wasn’t. We also expected that only one mutation would exist in this signalling pathway, and that also was wrong.”
The study appears April 1 in the early online edition of Cancer Discovery, a peer-reviewed journal of the American Association of Cancer Research.
About 50 percent of patients with metastatic melanoma, or 4,000 people a year, have the BRAF mutation and can be treated with the inhibitor Zelboraf — two pills taken twice daily. Zelboraf was approved by the U.S. Food and Drug Administration for use in metastatic melanoma in August 2011. Many other common human cancers, including colon, thyroid and lung cancers, also harbour BRAF-mutated subsets, Lo said.
According to Lo, the use of BRAF inhibitors leads to a response in about 60 percent of those with the mutation. After responding initially, however, most of those patients become resistant to the drug. Lo and his team of Jonsson Cancer Center scientists have been studying the mechanisms of resistance to see if they can either prevent it or find a way to re-sensitize the tumor to treatment. It was part of this work that led Lo to examine what role the MEK1 mutation might or might not be playing in that resistance.
“MEK1 is rarely mutated in cancers, but we found in this study that it was frequently associated with BRAF mutations,” Lo said. “The presence of both mutated MEK1 and BRAF might have been considered a biomarker for patients who would not respond to BRAF inhibitors. We were quite surprised when we found that patients with both mutations respond to BRAF inhibitors as well as those with only the BRAF mutation.”
In exploring the association between the two mutations, Lo and his team analyzed tumour samples from 31 melanoma patients treated with a BRAF inhibitor. Sixteen percent of the samples carried the double mutations before the cancer was treated, Lo said. The researchers’ findings were confirmed using melanoma cell lines grown in Lo’s laboratory.
Going forward, Lo and his team will look at approaches using inhibitors of MEK1 with BRAF inhibitors to determine if patients with the double mutations respond better and for longer periods. They will also try to understand why MEK1 mutations occur quite frequently in melanomas. About 15 percent of the patients with BRAF mutations also have a mutated MEK1, Lo said.
“As BRAF inhibitors gain widespread use for advanced melanoma treatment, biomarkers for drug sensitivity or resistance are urgently needed,” the study states. “We identify here concurrent activating mutations in BRAF and MEK1 in melanomas and show that the presence of a downstream mutation in MEK1 does not necessarily make BRAF mutant melanomas resistant to BRAF inhibitors.”
About 70,000 new cases of melanoma are diagnosed each year in the United States. Of those, 8,000 will die of the disease.