MYC is activated by USP2a-mediated modulation of microRNAs in prostate cancer

MYC 由前列腺癌中的 USP2a 介导的 microRNA 调节激活

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Significance

The deubiquitinating enzyme USP2a has previously been shown to be oncogenic, overexpressed in almost half of human prostate adenocarcinomas, and prolongs the half-life of targets such as fatty acid synthase, MDM2, and cyclin D1. Here, we highlight a new mechanism by which USP2a enhances MYC levels through the modulation of specific subsets of microRNAs in prostate cancer, suggesting alternative therapeutic strategies for targeting MYC.

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