ARID1A型
脱氮酶
泛素连接酶
泛素
癌症研究
生物
蛋白酶体
突变
细胞生物学
化学
生物化学
基因
作者
Qingyu Luo,Xiaowei Wu,Yabing Nan,Wan Chang,Pengfei Zhao,Yiping Zhang,Dan Su,Zhihua Liu
出处
期刊:Cell Reports
[Elsevier]
日期:2020-01-01
卷期号:30 (1): 98-111.e5
被引量:42
标识
DOI:10.1016/j.celrep.2019.12.017
摘要
Squamous cell carcinoma (SCC) is an aggressive epithelial malignancy, yet the molecular mechanisms underlying SCC development are elusive. ARID1A is frequently mutated in various cancer types, but both mutation rates and expression levels of ARID1A are ubiquitously low in SCCs. Here, we reveal that excessive protein degradation mediated by the ubiquitin-proteasome system (UPS) contributes to the loss of ARID1A expression in SCC. We identify that the E3 ligase TRIM32 and the deubiquitinase USP11 play key roles in controlling ARID1A stability. TRIM32 depletion inhibits SCC cell proliferation, metastasis, and chemoresistance by stabilizing ARID1A, while USP11 depletion promotes SCC development by promoting ARID1A degradation. We show that syndecan-2 (SDC2) is the downstream target of both ARID1A and USP11 and that SDC2 depletion abolishes the oncogenic function of ARID1A loss. In summary, our data reveal UPS-mediated protein degradation as a mechanism underlying ARID1A loss and propose an important role for the TRIM32/USP11-ARID1A-SDC2 axis in SCC.
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