Author:
Hostrup M,Lemminger AK,Stocks B,Gonzalez-Franquesa A,Larsen JK,Prats Quesada J,Thomassen M,Weinert BT,Bangsbo J,Deshmukh AS
Abstract
AbstractExercise is an effective strategy in the prevention and treatment of metabolic diseases. Alterations in the skeletal muscle proteome, including post-translational modifications, regulate its metabolic adaptations to exercise. Here, we examined the effect of high-intensity interval training (HIIT) on the proteome and acetylome of human skeletal muscle, revealing the response of 3168 proteins and 1263 lysine acetyl-sites on 464 acetylated proteins. We identified global protein adaptations to exercise training involved in metabolism, excitation-contraction coupling, and myofibrillar calcium sensitivity. Furthermore, HIIT increased the acetylation of mitochondrial proteins, particularly those of complex V. We also highlight the regulation of exercise-responsive histone acetyl-sites. These data demonstrate the plasticity of the skeletal muscle proteome and acetylome, providing insight into the regulation of contractile, metabolic and transcriptional processes within skeletal muscle. Herein, we provide a substantial hypothesis-generating resource to stimulate further mechanistic research investigating how exercise improves metabolic health.Impact statementHostrup and colleagues indentify global proteomic and acetylomic adaptations to high-intensity interval training, demonstrating apaptations to processes regulating metabolism and contraction.CONSORT flow diagram of enrolled participants
Publisher
Cold Spring Harbor Laboratory
Cited by
1 articles.
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