| Literature DB >> 33879767 |
Youqian Wu1, Chao Zhang2,3, Xiaolan Liu1, Zhengfu He4, Bing Shan5, Qingxin Zeng4, Qingwei Zhao1, Huaying Zhu6, Hongwei Liao7, Xufeng Cen1, Xiaoyan Xu1, Mengmeng Zhang5, Tingjun Hou8, Zhe Wang8, Huanhuan Yan1, Shuying Yang1, Yaqin Sun1, Yanying Chen1, Ronghai Wu1, Tingxue Xie1, Wei Chen6, Ayaz Najafov9, Songmin Ying10,11, Hongguang Xia12,13.
Abstract
Cancer expression of PD-L1 suppresses anti-tumor immunity. PD-L1 has emerged as a remarkable therapeutic target. However, the regulation of PD-L1 degradation is not understood. Here, we identify several compounds as inducers of PD-L1 degradation using a high-throughput drug screen. We find EGFR inhibitors promote PD-L1 ubiquitination and proteasomal degradation following GSK3α-mediated phosphorylation of Ser279/Ser283. We identify ARIH1 as the E3 ubiquitin ligase responsible for targeting PD-L1 to degradation. Overexpression of ARIH1 suppresses tumor growth and promotes cytotoxic T cell activation in wild-type, but not in immunocompromised mice, highlighting the role of ARIH1 in anti-tumor immunity. Moreover, combining EGFR inhibitor ES-072 with anti-CTLA4 immunotherapy results in an additive effect on both tumor growth and cytotoxic T cell activation. Our results delineate a mechanism of PD-L1 degradation and cancer escape from immunity via EGFR-GSK3α-ARIH1 signaling and suggest GSK3α and ARIH1 might be potential drug targets to boost anti-tumor immunity and enhance immunotherapies.Entities:
Year: 2021 PMID: 33879767 DOI: 10.1038/s41467-021-22467-8
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 14.919