Targeting Autophagy Sensitises Lung Cancer Cells to Src Family Kinase Inhibitors

Overview

Journal Oncotarget

Specialty Oncology

Date 2018 Jun 26

PMID 29937990

Citations 14

Authors

Ewa Rupniewska

Rajat Roy

Francesco A Mauri

Xinxue Liu

Maciej Kaliszczak

Guido Bellezza

Lucio Cagini

Mattia Barbareschi

Stefano Ferrero

Anna M Tommasi

Eric Aboagye

Michael J Seckl

Olivier E Pardo

Affiliations

Soon will be listed here.

Abstract

Lung cancer is the main cancer killer in both men and women, mostly due to the rapid development of drug resistant metastatic disease. Here, we evaluate the potential involvement of SRC family kinases (SFK) in lung cancer biology and assess the possible benefits of their inhibition as a therapeutic approach. We demonstrated that various SRC family members, including LYN and LCK, normally expressed solely in hematopoietic cells and neural tissues, are overexpressed and activated in a panel of SCLC and NSCLC cell lines. This was clinically relevant as LYN and FYN are also overexpressed in lung cancer clinical specimens. Moreover, LYN overexpression correlated with decreased patient survival on univariate and multivariate analysis. Dasatinib (BMS-354825), a SRC/ABL inhibitor, effectively blocked SFK activation at nanomolar concentrations which correlated with a significant decrease in cell numbers of multiple lung cancer cell lines. This effect was matched by a decrease in DNA synthesis, but only moderate induction of apoptosis. Indeed, dasatinib as well as PP2, another SFK inhibitor, strongly induced autophagy that likely prevented apoptosis. However, inhibition of this autophagic response induced robust apoptosis and sensitised lung cancer cells to dasatinib and . Our results provide an explanation for why dasatinib failed in NSCLC clinical trials. Furthermore, our data suggest that combining SFK inhibitors with autophagy inhibitors could provide a novel therapeutic approach in this disease.

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