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CHCHD4-TRIAP1 regulation of innate immune signaling mediates skeletal muscle adaptation to exercise

Jin Ma, Pingyuan Wang, Jie Zhuang, Annie Y. Son, Alexander Karius, Abu Mohammad Syed, Masahiro Nishi, Zhichao Wu, Mateus Prates Mori, Young‐Chae Kim, Paul M. Hwang

2023Cell Reports16 citationsDOIOpen Access PDF

Abstract

Exercise training can stimulate the formation of fatty-acid-oxidizing slow-twitch skeletal muscle fibers, which are inversely correlated with obesity, but the molecular mechanism underlying this transformation requires further elucidation. Here, we report that the downregulation of the mitochondrial disulfide relay carrier CHCHD4 by exercise training decreases the import of TP53-regulated inhibitor of apoptosis 1 (TRIAP1) into mitochondria, which can reduce cardiolipin levels and promote VDAC oligomerization in skeletal muscle. VDAC oligomerization, known to facilitate mtDNA release, can activate cGAS-STING/NFKB innate immune signaling and downregulate MyoD in skeletal muscle, thereby promoting the formation of oxidative slow-twitch fibers. In mice, CHCHD4 haploinsufficiency is sufficient to activate this pathway, leading to increased oxidative muscle fibers and decreased fat accumulation with aging. The identification of a specific mediator regulating muscle fiber transformation provides an opportunity to understand further the molecular underpinnings of complex metabolic conditions such as obesity and could have therapeutic implications.

Topics & Concepts

Skeletal muscleCell biologyDownregulation and upregulationInnate immune systemMediatorMitochondrionChemistryOxidative phosphorylationBiologyEndocrinologyBiochemistryReceptorGeneinterferon and immune responsesUbiquitin and proteasome pathwaysAdipose Tissue and Metabolism
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