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Cytochrome c lysine acetylation regulates cellular respiration and cell death in ischemic skeletal muscle

Authors :
Universidad de Sevilla. Departamento de Química Física
Universidad de Sevilla. Departamento de Bioquímica Vegetal y Biología Molecular
National Institutes of Health. United States
Ministerio de Ciencia e Innovación (MICIN). España
Junta de Andalucía
Morse, Paul T.
Pérez Mejías, Gonzalo
Wan, Junmei
Turner, Alice A.
Márquez Escudero, Inmaculada
Kalpage, Hasini A.
Vaishnav, Asmita
Zurek, Matthew P.
Huettemann, Philipp P.
Kim, Katherine
Arroum, Tasnim
Rosa Acosta, Miguel Ángel de la
Chowdhury, Dipanwita Dutta
Díaz Moreno, Irene
Hüttemann, Maik
Universidad de Sevilla. Departamento de Química Física
Universidad de Sevilla. Departamento de Bioquímica Vegetal y Biología Molecular
National Institutes of Health. United States
Ministerio de Ciencia e Innovación (MICIN). España
Junta de Andalucía
Morse, Paul T.
Pérez Mejías, Gonzalo
Wan, Junmei
Turner, Alice A.
Márquez Escudero, Inmaculada
Kalpage, Hasini A.
Vaishnav, Asmita
Zurek, Matthew P.
Huettemann, Philipp P.
Kim, Katherine
Arroum, Tasnim
Rosa Acosta, Miguel Ángel de la
Chowdhury, Dipanwita Dutta
Díaz Moreno, Irene
Hüttemann, Maik
Publication Year :
2023

Abstract

Skeletal muscle is more resilient to ischemia-reperfusion injury than other organs. Tissue specific post-translational modifications of cytochrome c (Cytc) are involved in ischemia-reperfusion injury by regulating mitochondrial respiration and apoptosis. Here, we describe an acetylation site of Cytc, lysine 39 (K39), which was mapped in ischemic porcine skeletal muscle and removed by sirtuin5 in vitro. Using purified protein and cellular double knockout models, we show that K39 acetylation and acetylmimetic K39Q replacement increases cytochrome c oxidase (COX) activity and ROS scavenging while inhibiting apoptosis via decreased binding to Apaf-1, caspase cleavage and activity, and cardiolipin peroxidase activity. These results are discussed with X-ray crystallography structures of K39 acetylated (1.50 Å) and acetylmimetic K39Q Cytc (1.36 Å) and NMR dynamics. We propose that K39 acetylation is an adaptive response that controls electron transport chain flux, allowing skeletal muscle to meet heightened energy demand while simultaneously providing the tissue with robust resilience to ischemia-reperfusion injury.

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1458411175
Document Type :
Electronic Resource

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