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USP11 promotes prostate cancer progression by up-regulating AR and c-Myc activity.


ABSTRACT: Androgen receptor (AR) is a main driver for castration-resistant prostate cancer (CRPC). c-Myc is an oncogene underlying prostate tumorigenesis. Here, we find that the deubiquitinase USP11 targets both AR and c-Myc in prostate cancer (PCa). USP11 expression was up-regulated in metastatic PCa and CRPC. USP11 knockdown (KD) significantly inhibited PCa cell growth. Our RNA-seq studies revealed AR and c-Myc as the top transcription factors altered after USP11 KD. ChIP-seq analysis showed that either USP11 KD or replacement of endogenous USP11 with a catalytic-inactive USP11 mutant significantly decreased chromatin binding by AR and c-Myc. We find that USP11 employs two mechanisms to up-regulate AR and c-Myc levels: namely, deubiquitination of AR and c-Myc proteins to increase their stability and deubiquitination of H2A-K119Ub, a repressive histone mark, on promoters of AR and c-Myc genes to increase their transcription. AR and c-Myc reexpression in USP11-KD PCa cells partly rescued cell growth defects. Thus, our studies reveal a tumor-promoting role for USP11 in aggressive PCa through upregulation of AR and c-Myc activities and support USP11 as a potential target against PCa.

SUBMITTER: Pornour M 

PROVIDER: S-EPMC11295044 | biostudies-literature | 2024 Jul

REPOSITORIES: biostudies-literature

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USP11 promotes prostate cancer progression by up-regulating AR and c-Myc activity.

Pornour Majid M   Jeon Hee-Young HY   Ryu Hyunju H   Khadka Sudeep S   Xu Rui R   Chen Hegang H   Hussain Arif A   Lam Hung-Ming HM   Zhuang Zhihao Z   Oo Htoo Zarni HZ   Gleave Martin M   Dong Xuesen X   Wang Qianben Q   Barbieri Christopher C   Qi Jianfei J  

Proceedings of the National Academy of Sciences of the United States of America 20240725 31


Androgen receptor (AR) is a main driver for castration-resistant prostate cancer (CRPC). c-Myc is an oncogene underlying prostate tumorigenesis. Here, we find that the deubiquitinase USP11 targets both AR and c-Myc in prostate cancer (PCa). USP11 expression was up-regulated in metastatic PCa and CRPC. USP11 knockdown (KD) significantly inhibited PCa cell growth. Our RNA-seq studies revealed AR and c-Myc as the top transcription factors altered after USP11 KD. ChIP-seq analysis showed that either  ...[more]

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