Mitochondrial dysfunction in skeletal muscle contributes to the development of acute insulin resistance in mice

Hyunjung Lee; Tae Youl Ha; Chang Hwa Jung; Farida Sukma Nirmala; So‐Young Park; Yang Hoon Huh; Jiyun Ahn

doi:10.1002/jcsm.12794

Journal of Cachexia, Sarcopenia and Muscle (Dec 2021)

Mitochondrial dysfunction in skeletal muscle contributes to the development of acute insulin resistance in mice

Hyunjung Lee,
Tae Youl Ha,
Chang Hwa Jung,
Farida Sukma Nirmala,
So‐Young Park,
Yang Hoon Huh,
Jiyun Ahn

Affiliations

Hyunjung Lee: Research Group of Natural Material and Metabolism Korea Food Research Institute Wanju Republic of Korea
Tae Youl Ha: Research Group of Natural Material and Metabolism Korea Food Research Institute Wanju Republic of Korea
Chang Hwa Jung: Research Group of Natural Material and Metabolism Korea Food Research Institute Wanju Republic of Korea
Farida Sukma Nirmala: Research Group of Natural Material and Metabolism Korea Food Research Institute Wanju Republic of Korea
So‐Young Park: Department of Physiology, College of Medicine Yeungnam University Daegu Republic of Korea
Yang Hoon Huh: Center for Electron Microscopy Research Korea Basic Science Institute Cheongju Republic of Korea
Jiyun Ahn: Research Group of Natural Material and Metabolism Korea Food Research Institute Wanju Republic of Korea

DOI: https://doi.org/10.1002/jcsm.12794
Journal volume & issue: Vol. 12, no. 6
pp. 1925 – 1939

Abstract

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Abstract Background Although mounting evidence indicates that insulin resistance (IR) co‐occurs with mitochondrial dysfunction in skeletal muscle, there is no clear causal link between mitochondrial dysfunction and IR pathogenesis. In this study, the exact role of mitochondria in IR development was determined. Methods Six‐week‐old C57BL/6 mice were fed a high‐fat diet for 2 weeks to induce acute IR or for 24 weeks to induce chronic IR (n = 8 per group). To characterize mitochondrial function, we measured citrate synthase activity, ATP content, mitochondrial DNA (mtDNA) content, and oxygen consumption rate in gastrocnemius and liver tissues. We intraperitoneally administered mitochondrial division inhibitor 1 (mdivi‐1) to mice with acute IR and measured mitochondrial adaptive responses such as mitophagy, mitochondrial unfolded protein response (UPRmt), and oxidative stress (n = 6 per group). Results Acute IR occurred coincidently with impaired mitochondrial function, including reduced citrate synthase activity (−37.8%, P < 0.01), ATP production (−88.0%, P < 0.01), mtDNA (−53.1%, P < 0.01), and mitochondrial respiration (−52.2% for maximal respiration, P < 0.05) in skeletal muscle but not in liver. Administration of mdivi‐1 attenuated IR development by increasing mitochondrial function (+58.5% for mtDNA content, P < 0.01; 4.06 ± 0.69 to 5.84 ± 0.95 pmol/min/mg for citrate synthase activity, P < 0.05; 13.06 ± 0.70 to 34.87 ± 0.70 pmol/min/g for maximal respiration, P < 0.001). Western blot analysis showed acute IR resulted in increased autophagy (mitophagy) and UPRmt induction in muscle tissue. This adaptive response was inhibited by mdivi‐1, which reduced the mitochondrial oxidative stress of skeletal muscle during acute IR. Conclusions Acute IR induced mitochondrial oxidative stress that impaired mitochondrial function in skeletal muscle. Improving mitochondrial function has important potential for treating acute IR.

Published in Journal of Cachexia, Sarcopenia and Muscle

ISSN: 2190-5991 (Print); 2190-6009 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the musculoskeletal system; Science: Human anatomy
Website: https://onlinelibrary.wiley.com/journal/1353921906009

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