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The interplay between SUMOylation and phosphorylation of PKCδ facilitates oxidative stress‐induced apoptosis

Siman Gao, Xiangteng Zhao, Lin Hou, Ruining Ma, Jie Zhou, Michael X. Zhu, Si‐Jian Pan, Yong Li

2021FEBS Journal12 citationsDOIOpen Access PDF

Abstract

Although the increase in the number of identified posttranslational modifications (PTMs) has substantially improved our knowledge about substrate site specificity of single PTMs, the fact that different types of PTMs can crosstalk and act in concert to exert important regulatory mechanisms for protein function has not gained much attention. Here, we show that protein kinase Cδ (PKCδ) is SUMOylated at lysine 473 in its C‐terminal catalytic domain, and the SUMOylation increases PKCδ stability by repressing its ubiquitination. In addition, we uncover a functional interplay between the phosphorylation and SUMOylation of PKCδ, which can strengthen each other through recruiting SUMO E2/E3 ligases and the PKCδ kinase, respectively, to the PKCδ complexes. We identified PIAS2β as the SUMO E3 ligase of PKCδ. More importantly, by enhancing PKCδ protein stability and its phosphorylation through an interdependent interplay of the PTMs, the SUMOylation of PKCδ promotes apoptotic cell death induced by H 2 O 2 . We conclude that SUMOylation represents an important regulatory mechanism of PKCδ PTMs for the kinase's function in oxidative cell damage.

Topics & Concepts

SUMO proteinProtein kinase CPhosphorylationCell biologyUbiquitinCrosstalkUbiquitin ligaseNEDD8LysineKinaseBiologyChemistryBiochemistryAmino acidGeneOpticsPhysicsUbiquitin and proteasome pathwaysCancer-related Molecular PathwaysPeptidase Inhibition and Analysis