CFLIP Suppression and DR5 Activation Sensitize Senescent Cancer Cells to Senolysis

Overview

Journal Nat Cancer

Specialty Oncology

Date 2022 Nov 22

PMID 36414711

Authors

Liqin Wang

Haojie Jin

Fleur Jochems

Siying Wang

Cor Lieftink

Isabel Mora Martinez

Giulia De Conti

Finn Edwards

Rodrigo Leite de Oliveira

Arnout Schepers

Yangyang Zhou

Jiaojiao Zheng

Wei Wu

Xingling Zheng

Shengxian Yuan

Jing Ling

Kathy Jastrzebski

Matheus Dos Santos Dias

Ji-Ying Song

Patrick N H Celie

Hideo Yagita

Ming Yao

Weiping Zhou

Roderick L Beijersbergen

Wenxin Qin

Rene Bernards

Affiliations

Soon will be listed here.

Abstract

Senolytics, drugs that kill senescent cells, have been proposed to improve the response to pro-senescence cancer therapies; however, this remains challenging due to a lack of broadly acting senolytic drugs. Using CRISPR/Cas9-based genetic screens in different senescent cancer cell models, we identify loss of the death receptor inhibitor cFLIP as a common vulnerability of senescent cancer cells. Senescent cells are primed for apoptotic death by NF-κB-mediated upregulation of death receptor 5 (DR5) and its ligand TRAIL, but are protected from death by increased cFLIP expression. Activation of DR5 signaling by agonistic antibody, which can be enhanced further by suppression of cFLIP by BRD2 inhibition, leads to efficient killing of a variety of senescent cancer cells. Moreover, senescent cells sensitize adjacent non-senescent cells to killing by DR5 agonist through a bystander effect mediated by secretion of cytokines. We validate this 'one-two punch' cancer therapy by combining pro-senescence therapy with DR5 activation in different animal models.

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