Targeting Autophagy Inhibits Melanoma Growth by Enhancing NK Cells Infiltration in a CCL5-dependent Manner

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2017 Oct 29

PMID 29078276

Citations 134

Authors

Takouhie Mgrditchian

Tsolere Arakelian

Jerome Paggetti

Muhammad Zaeem Noman

Elodie Viry

Etienne Moussay

Kris Van Moer

Stephanie Kreis

Coralie Guerin

Stephanie Buart

Caroline Robert

Christophe Borg

Philippe Vielh

Salem Chouaib

Guy Berchem

Bassam Janji

Affiliations

Soon will be listed here.

Abstract

While blocking tumor growth by targeting autophagy is well established, its role on the infiltration of natural killer (NK) cells into tumors remains unknown. Here, we investigate the impact of targeting autophagy gene Beclin1 () on the infiltration of NK cells into melanomas. We show that, in addition to inhibiting tumor growth, targeting increased the infiltration of functional NK cells into melanoma tumors. We provide evidence that driving NK cells to the tumor bed relied on the ability of autophagy-defective tumors to transcriptionally overexpress the chemokine gene Such infiltration and tumor regression were abrogated by silencing CCL5 in BECN1-defective tumors. Mechanistically, we show that the up-regulated expression of CCL5 occurred through the activation of its transcription factor c-Jun by a mechanism involving the impairment of phosphatase PP2A catalytic activity and the subsequent activation of JNK. Similar to , targeting other autophagy genes, such as , /, or inhibiting autophagy pharmacologically by chloroquine, also induced the expression of in melanoma cells. Clinically, a positive correlation between CCL5 and NK cell marker NKp46 expression was found in melanoma patients, and a high expression level of CCL5 was correlated with a significant improvement of melanoma patients' survival. We believe that this study highlights the impact of targeting autophagy on the tumor infiltration by NK cells and its benefit as a novel therapeutic approach to improve NK-based immunotherapy.

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