Targeting Autophagy Peptidase ATG4B with a Novel Natural Product Inhibitor Azalomycin F4a for Advanced Gastric Cancer

Overview

Journal Cell Death Dis

Specialties Cell Biology
General Medicine

Date 2022 Feb 20

PMID 35184132

Authors

Lin Zhong

Bin Yang

Zhenhua Zhang

Junfeng Wang

Xiaojuan Wang

Yinfeng Guo

Weifeng Huang

Qianqian Wang

Guodi Cai

Fan Xia

Shengning Zhou

Shuai Ma

Yichu Nie

Jinping Lei

Min Li

Peiqing Liu

Wenbin Deng

Yonghong Liu

Fanghai Han

Junjian Wang

Affiliations

Soon will be listed here.

Abstract

Advanced gastric cancer (GCa) remains highly lethal due to the lack of effective therapies. Identifying promising therapeutic targets and developing effective treatment against GCa are urgently needed. Through mRNA and protein analysis of GCa clinical tumor samples, we found that autophagy-related gene 4B (ATG4B) was overexpressed in GCa tumors and that its high expression was associated with patients' poor prognosis. Knockdown of ATG4B significantly inhibited GCa cell survival and tumor growth. To further probe the role of ATG4B in GCa by pharmacological means, we screened an in-house marine natural compound library against ATG4B and identified Azalomycin F4a (Am-F4a) as a novel and potent ATG4B inhibitor. Am-F4a directly bound to ATG4B with high affinity and effectively suppressed GCa cell autophagy via inhibition of ATG4B both in vitro and in vivo. Moreover, Am-F4a or ATG4B knockdown significantly suppressed tumor growth as well as GCa cell migration and invasion. Am-F4a effectively blocked the metastatic progression of primary GCa and sensitized tumors to chemotherapy. Taken together, our findings indicate that ATG4B is a potential therapeutic target against GCa and the natural product Am-F4a is a novel ATG4B inhibitor that can be further developed for the treatment of GCa.

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