![](\"https:\/\/www.infobioquimica.com\/new\/wp-content\/uploads\/2017\/08\/Prostate-cancer-figure-e1502382186725-1024x525.png\")
<\/a><\/p>\nIn the publication, the authors explain the role of mutations within the SPOP gene on the development of resistance to one class of drugs. SPOP mutations are the most frequent genetic changes seen in primary prostate cancer. These mutations play a central role in the development of resistance to drugs called BET-inhibitors.<\/p>\n
BET, bromodomain and extra-terminal domain, inhibitors are drugs that prevent the action of BET proteins. These proteins help guide the abnormal growth of cancer cells.<\/p>\n
As a therapy, BET-inhibitors are promising, but drug resistance often develops, says Haojie Huang Ph.D., senior author and a molecular biologist within Mayo Clinic\u2019s Center for Biomedical Discovery. Prostate cancer is among the most diagnosed malignancies in the United States. It is also the third leading cause of cancer death in American men, according to the American Cancer Society. Because of this, says Dr. Huang, improving treatments for prostate cancer is an important public health goal.<\/p>\n
In the publication, the authors report SPOP mutations stabilize BET proteins against the action of BET-inhibitors. By this action, the mutations also promote cancer cell proliferation, invasion and survival.<\/p>\n
\u201cThese findings have important implications for prostate cancer treatment, because SPOP mutation or elevated BET protein expression can now be used as biomarkers to improve outcome of BET inhibitor-oriented therapy of prostate cancer with SPOP mutation or BET protein overexpression,\u201d says Dr. Huang.<\/p>\n
Mutations in the SPOP gene (depicted on the left, below) can then be used to guide administration of anti-cancer drugs (labeled treatment A through D below) in patients with prostate cancer:<\/p>\n
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