Inter-organellar and Systemic Responses to Impaired Mitochondrial Matrix Protein Import in Skeletal Muscle

Overview

Journal Commun Biol

Specialty Biology

Date 2022 Oct 5

PMID 36198903

Authors

Nirajan Neupane

Jayasimman Rajendran

Jouni Kvist

Sandra Harjuhaahto

Bowen Hu

Veijo Kinnunen

Yang Yang

Anni I Nieminen

Henna Tyynismaa

Affiliations

Soon will be listed here.

Abstract

Effective protein import from cytosol is critical for mitochondrial functions and metabolic regulation. We describe here the mammalian muscle-specific and systemic consequences to disrupted mitochondrial matrix protein import by targeted deletion of the mitochondrial HSP70 co-chaperone GRPEL1. Muscle-specific loss of GRPEL1 caused rapid muscle atrophy, accompanied by shut down of oxidative phosphorylation and mitochondrial fatty acid oxidation, and excessive triggering of proteotoxic stress responses. Transcriptome analysis identified new responders to mitochondrial protein import toxicity, such as the neurological disease-linked intermembrane space protein CHCHD10. Besides communication with ER and nucleus, we identified crosstalk of distressed mitochondria with peroxisomes, in particular the induction of peroxisomal Acyl-CoA oxidase 2 (ACOX2), which we propose as an ATF4-regulated peroxisomal marker of integrated stress response. Metabolic profiling indicated fatty acid enrichment in muscle, a shift in TCA cycle intermediates in serum and muscle, and dysregulated bile acids. Our results demonstrate the fundamental importance of GRPEL1 and provide a robust model for detecting mammalian inter-organellar and systemic responses to impaired mitochondrial matrix protein import and folding.

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