CRIF1 As a Potential Target to Improve the Radiosensitivity of Osteosarcoma

Overview

Journal Proc Natl Acad Sci U S A

Specialty Science

Date 2019 Sep 25

PMID 31548420

Citations 12

Authors

Qian Ran

Feng Jin

Yang Xiang

Lixin Xiang

Qiushi Wang

Fengjie Li

Li Chen

Yuan Zhang

Chun Wu

Luping Zhou

Yanni Xiao

Lili Chen

Jiang Wu

Jiang F Zhong

Shengwen Calvin Li

Zhongjun Li

Affiliations

Soon will be listed here.

Abstract

Resistance to ionizing radiation (IR), which is a conventional treatment for osteosarcoma that cannot be resected, undermines the efficacy of this therapy. However, the mechanism by which IR induces radioresistance in osteosarcoma is not defined. Here, we report that CR6-interacting factor-1 (CRIF1) is highly expressed in osteosarcoma and undergoes nuclear-cytoplasmic shuttling of cyclin-dependent kinase 2 (CDK2) after IR. Osteosarcoma cells lacking CRIF1 show increased sensitivity to IR, which is associated with delayed DNA damage repair, inactivated G1/S checkpoint, and mitochondrial dysfunction. CRIF1 interacts with the DNA damage checkpoint regulator CDK2, and CRIF1 and CDK2 colocalize in the nucleus after IR. Nuclear localization of CDK2 is associated with phosphorylation changes that promote DNA repair and activation of the G1/S checkpoint. CRIF1 knockdown synergized with IR in an in vivo osteosarcoma model, leading to tumor regression. Based on these findings, we identify CRIF1 as a potential therapeutic target in osteosarcoma that can increase the efficacy of radiotherapy. More broadly, our findings may provide insights into the mechanism for other types of radioresistant cancers and be exploited for therapeutic ends.

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