Transient Targeting of BIM-dependent Adaptive MCL1 Preservation Enhances Tumor Response to Molecular Therapeutics in Non-small Cell Lung Cancer

Overview

Journal Cell Death Differ

Specialty Cell Biology

Date 2022 Sep 28

PMID 36171331

Authors

Kaixuan Shi

Haijiao Lu

Zhenfeng Zhang

Yujie Fu

Jie Wu

Shichao Zhou

Pengfei Ma

Kaiyan Ye

Shengzhe Zhang

Hailei Shi

Weiping Shi

Mei-Chun Cai

Xiaojing Zhao

Zhuang Yu

Jian Tang

Guanglei Zhuang

Affiliations

Soon will be listed here.

Abstract

Despite remarkable efficacy, targeted treatments often yield a subpopulation of residual tumor cells in part due to non-genetic adaptions. Previous mechanistic understanding on the emergence of these drug-tolerant persisters (DTPs) has been limited to epigenetic and transcriptional reprogramming. Here, by comprehensively interrogating therapy-induced early dynamic protein changes in diverse oncogene-addicted non-small cell lung cancer models, we identified adaptive MCL1 increase as a new and universal mechanism to confer apoptotic evasion and DTP formation. In detail, acute MAPK signaling disruption in the presence of genotype-based tyrosine kinase inhibitors (TKIs) prompted mitochondrial accumulation of pro-apoptotic BH3-only protein BIM, which sequestered MCL1 away from MULE-mediated degradation. A small-molecule combination screen uncovered that PI3K-mTOR pathway blockade prohibited MCL1 upregulation. Biochemical and immunocytochemical evidence indicated that mTOR complex 2 (mTORC2) bound and phosphorylated MCL1, facilitating its interaction with BIM. As a result, short-term polytherapy combining antineoplastic TKIs with PI3K, mTOR or MCL1 inhibitors sufficed to prevent DTP development and promote cancer eradication. Collectively, these findings support that upfront and transient targeting of BIM-dependent, mTORC2-regulated adaptive MCL1 preservation holds enormous promise to improve the therapeutic index of molecular targeted agents.

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