DRP1-mediated mitochondrial shape controls calcium homeostasis and muscle mass

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作者
Giulia Favaro
Vanina Romanello
Tatiana Varanita
Maria Andrea Desbats
Valeria Morbidoni
Caterina Tezze
Mattia Albiero
Marta Canato
Gaia Gherardi
Diego De Stefani
Cristina Mammucari
Bert Blaauw
Simona Boncompagni
Feliciano Protasi
Carlo Reggiani
Luca Scorrano
Leonardo Salviati
Marco Sandri
机构
[1] Venetian Institute of Molecular Medicine,Department of Biomedical Science
[2] University of Padova,Myology Center
[3] University of Padova,Department of Biology
[4] University of Padova,Clinical Genetics Unit, Department of Woman and Child Health
[5] University of Padova,Department of Medicine
[6] IRP Città della Speranza Corso Stati Uniti 4, DIMED
[7] University of Padova,Center for Research on Ageing and Translational Medicine (CeSI
[8] via Luigi Polacchi,MeT))
[9] University G. d’ Annunzio,Institute for Kinesiology Research
[10] Science and Research Center of Koper,Department of Medicine
[11] McGill University,undefined
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摘要
Mitochondrial quality control is essential in highly structured cells such as neurons and muscles. In skeletal muscle the mitochondrial fission proteins are reduced in different physiopathological conditions including ageing sarcopenia, cancer cachexia and chemotherapy-induced muscle wasting. However, whether mitochondrial fission is essential for muscle homeostasis is still unclear. Here we show that muscle-specific loss of the pro-fission dynamin related protein (DRP) 1 induces muscle wasting and weakness. Constitutive Drp1 ablation in muscles reduces growth and causes animal death while inducible deletion results in atrophy and degeneration. Drp1 deficient mitochondria are morphologically bigger and functionally abnormal. The dysfunctional mitochondria signals to the nucleus to induce the ubiquitin-proteasome system and an Unfolded Protein Response while the change of mitochondrial volume results in an increase of mitochondrial Ca2+ uptake and myofiber death. Our findings reveal that morphology of mitochondrial network is critical for several biological processes that control nuclear programs and Ca2+ handling.
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