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Inhibition of c-MET upregulates PD-L1 expression in lung adenocarcinoma.

Xian Wen Sun, Chia-Wei Li, Wei‐Jan Wang, Mei‐Kuang Chen, Hui Li, Yun‐Ju Lai, Jennifer L. Hsu, Paul Koller, Li-Chuan Chan, Pei‐Chih Lee, Fang‐Ju Cheng, Clinton Yam, Gongyan Chen, Mien‐Chie Hung

2020PubMed29 citationsOpen Access PDF

Abstract

Non-small cell lung cancer (NSCLC) patients with c-MET dysregulation may benefit from c-MET inhibitors therapy as inhibition of c-MET activity has emerged as a therapeutic approach against this disease. Although several c-MET inhibitors have been evaluated in multiple clinical trials in lung cancer, their benefits so far have been modest. Thus, furthering our understanding of the mechanisms contributing to the lack of success of c-MET inhibitors in clinical trials is essential toward the development of rational and effective combination strategies. Here we show that exposure of NCSLC cell lines to c-MET inhibitor tivantinib increases their expression of PD-L1, which in turn causes cells to become more resistant to T-cell killing. Mechanistically, inhibition of c-MET suppresses p-GSK3β, leading to the stabilization of PD-L1 similar to that observed in liver cancer cells. Collectively, our findings suggest a potential crosstalk between c-MET inhibition and immune escape and provide a rationale for the combination therapy of c-MET inhibitors and immune checkpoint blockade in NSCLC.

Topics & Concepts

Cancer researchLung cancerBlockadeClinical trialMedicineCrosstalkImmunotherapyImmune systemC-MetPD-L1AdenocarcinomaCancerPharmacologyOncologyInternal medicineImmunologyReceptorOpticsPhysicsHepatocyte growth factorLiver physiology and pathology
Inhibition of c-MET upregulates PD-L1 expression in lung adenocarcinoma. | Litcius