PRL2 serves as a negative regulator in cell adaptation to oxidative stress

Xinyue Du; Yang Zhang; Xiao Li; Qi Li; Chenyun Wu; Guangjie Chen; XiaoKui Guo; Yongqiang Weng; Zhaojun Wang

doi:10.1186/s13578-019-0358-z

PRL2 serves as a negative regulator in cell adaptation to oxidative stress

Cell Biosci. 2019 Nov 29:9:96. doi: 10.1186/s13578-019-0358-z. eCollection 2019.

Authors

Xinyue Du^#¹, Yang Zhang^#¹, Xiao Li¹, Qi Li¹, Chenyun Wu¹, Guangjie Chen¹, XiaoKui Guo², Yongqiang Weng³, Zhaojun Wang¹

Affiliations

¹ 1Department of Immunology and Microbiology, Shanghai Jiao Tong University School of Medicine, Rm 709 Bldg 5, 280 S. Chongqing Rd, Shanghai, 200025 People's Republic of China.
² 3Institute for Global Health, Shanghai Jiao Tong University School of Medicine-Chinese Center for Tropical Diseases Research, Shanghai, 200025 People's Republic of China.
³ 2Department of General Surgery, Huadong Hospital, Shanghai Medical College, Fudan University, Shanghai, 200040 People's Republic of China.

^# Contributed equally.

Abstract

High levels of ROS cause oxidative stress, which plays a critical role in cell death. As a ROS effector protein, PRL2 senses ROS and controls phagocyte bactericidal activity during infection. Here we report PRL2 regulates oxidative stress induced cell death. PRL2 senses oxidative stress via highly reactive cysteine residues at 46 and 101. The oxidation of PRL2 causes protein degradation and supports pro-survival PDK1/AKT signal which in turn to protect cells against oxidative stress. As a result, PRL2 levels have a high correlation with oxidative stress induced cell death. In vivo experiments showed PRL2 deficient cells survive better in inflammatory oxidative environment and resist to ionizing radiation. Our finding suggests PRL2 serves as a negative regulator in cell adaptation to oxidative stress. Therefore, PRL2 could be targeted to modulate cell viability in inflammation or irradiation associated therapy.

Keywords: Cell death; Inflammation; Ionizing radiation; Oxidative stress; PRL2.