4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia

BACKGROUND: Sarcopenia is the loss of muscle mass/function that occurs during the aging process. The links between mechanistic target of rapamycin (mTOR) activity and muscle development are largely documented, but the role of its downstream targets in the development of sarcopenia is poorly understo...

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Autores principales: Le Bacquer, Olivier, Combe, Kristell, Patrac, Véronique, Ingram, Brian, Combaret, Lydie, Dardevet, Dominique, Montaurier, Christophe, Salles, Jérôme, Giraudet, Christophe, Guillet, Christelle, Sonenberg, Nahum, Boirie, Yves, Walrand, Stéphane
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
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Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6596930/
https://www.ncbi.nlm.nih.gov/pubmed/30927336
http://dx.doi.org/10.1002/jcsm.12412
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author Le Bacquer, Olivier
Combe, Kristell
Patrac, Véronique
Ingram, Brian
Combaret, Lydie
Dardevet, Dominique
Montaurier, Christophe
Salles, Jérôme
Giraudet, Christophe
Guillet, Christelle
Sonenberg, Nahum
Boirie, Yves
Walrand, Stéphane
author_facet Le Bacquer, Olivier
Combe, Kristell
Patrac, Véronique
Ingram, Brian
Combaret, Lydie
Dardevet, Dominique
Montaurier, Christophe
Salles, Jérôme
Giraudet, Christophe
Guillet, Christelle
Sonenberg, Nahum
Boirie, Yves
Walrand, Stéphane
author_sort Le Bacquer, Olivier
collection PubMed
description BACKGROUND: Sarcopenia is the loss of muscle mass/function that occurs during the aging process. The links between mechanistic target of rapamycin (mTOR) activity and muscle development are largely documented, but the role of its downstream targets in the development of sarcopenia is poorly understood. Eukaryotic initiation factor 4E‐binding proteins (4E‐BPs) are targets of mTOR that repress mRNA translation initiation and are involved in the control of several physiological processes. However, their role in skeletal muscle is still poorly understood. The goal of this study was to assess how loss of 4E‐BP1 and 4E‐BP2 expression impacts skeletal muscle function and homeostasis in aged mice and to characterize the associated metabolic changes by metabolomic and lipidomic profiling. METHODS: Twenty‐four‐month‐old wild‐type and whole body 4E‐BP1/4E‐BP2 double knockout (DKO) mice were used to measure muscle mass and function. Protein homeostasis was measured ex vivo in extensor digitorum longus by incorporation of l‐[U‐(14)C]phenylalanine, and metabolomic and lipidomic profiling of skeletal muscle was performed by Metabolon, Inc. RESULTS: The 4E‐BP1/2 DKO mice exhibited an increase in muscle mass that was associated with increased grip strength (P < 0.05). Protein synthesis was higher under both basal (+102%, P < 0.05) and stimulated conditions (+65%, P < 0.05) in DKO skeletal muscle. Metabolomic and complex lipid analysis of skeletal muscle revealed robust differences pertaining to amino acid homeostasis, carbohydrate abundance, and certain aspects of lipid metabolism. In particular, levels of most free amino acids were lower within the 4E‐BP1/2 DKO muscle. Interestingly, although glucose levels were unchanged, differences were observed in the isobaric compound maltitol/lactitol (33‐fold increase, P < 0.01) and in several additional carbohydrate compounds. 4E‐BP1/2 depletion also resulted in accumulation of medium‐chain acylcarnitines and a 20% lower C2/C0 acylcarnitine ratio (P < 0.01) indicative of reduced β‐oxidation. CONCLUSIONS: Taken together, these findings demonstrate that deletion of 4E‐BPs is associated with perturbed energy metabolism in skeletal muscle and could have beneficial effects on skeletal muscle mass and function in aging mice. They also identify 4E‐BPs as potential targets for the treatment of sarcopenia.
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spelling pubmed-65969302019-07-11 4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia Le Bacquer, Olivier Combe, Kristell Patrac, Véronique Ingram, Brian Combaret, Lydie Dardevet, Dominique Montaurier, Christophe Salles, Jérôme Giraudet, Christophe Guillet, Christelle Sonenberg, Nahum Boirie, Yves Walrand, Stéphane J Cachexia Sarcopenia Muscle Original Articles BACKGROUND: Sarcopenia is the loss of muscle mass/function that occurs during the aging process. The links between mechanistic target of rapamycin (mTOR) activity and muscle development are largely documented, but the role of its downstream targets in the development of sarcopenia is poorly understood. Eukaryotic initiation factor 4E‐binding proteins (4E‐BPs) are targets of mTOR that repress mRNA translation initiation and are involved in the control of several physiological processes. However, their role in skeletal muscle is still poorly understood. The goal of this study was to assess how loss of 4E‐BP1 and 4E‐BP2 expression impacts skeletal muscle function and homeostasis in aged mice and to characterize the associated metabolic changes by metabolomic and lipidomic profiling. METHODS: Twenty‐four‐month‐old wild‐type and whole body 4E‐BP1/4E‐BP2 double knockout (DKO) mice were used to measure muscle mass and function. Protein homeostasis was measured ex vivo in extensor digitorum longus by incorporation of l‐[U‐(14)C]phenylalanine, and metabolomic and lipidomic profiling of skeletal muscle was performed by Metabolon, Inc. RESULTS: The 4E‐BP1/2 DKO mice exhibited an increase in muscle mass that was associated with increased grip strength (P < 0.05). Protein synthesis was higher under both basal (+102%, P < 0.05) and stimulated conditions (+65%, P < 0.05) in DKO skeletal muscle. Metabolomic and complex lipid analysis of skeletal muscle revealed robust differences pertaining to amino acid homeostasis, carbohydrate abundance, and certain aspects of lipid metabolism. In particular, levels of most free amino acids were lower within the 4E‐BP1/2 DKO muscle. Interestingly, although glucose levels were unchanged, differences were observed in the isobaric compound maltitol/lactitol (33‐fold increase, P < 0.01) and in several additional carbohydrate compounds. 4E‐BP1/2 depletion also resulted in accumulation of medium‐chain acylcarnitines and a 20% lower C2/C0 acylcarnitine ratio (P < 0.01) indicative of reduced β‐oxidation. CONCLUSIONS: Taken together, these findings demonstrate that deletion of 4E‐BPs is associated with perturbed energy metabolism in skeletal muscle and could have beneficial effects on skeletal muscle mass and function in aging mice. They also identify 4E‐BPs as potential targets for the treatment of sarcopenia. John Wiley and Sons Inc. 2019-03-29 2019-06 /pmc/articles/PMC6596930/ /pubmed/30927336 http://dx.doi.org/10.1002/jcsm.12412 Text en © 2019 The Authors. Journal of Cachexia, Sarcopenia and Muscle published by John Wiley & Sons Ltd on behalf of the Society on Sarcopenia, Cachexia and Wasting Disorders This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Original Articles
Le Bacquer, Olivier
Combe, Kristell
Patrac, Véronique
Ingram, Brian
Combaret, Lydie
Dardevet, Dominique
Montaurier, Christophe
Salles, Jérôme
Giraudet, Christophe
Guillet, Christelle
Sonenberg, Nahum
Boirie, Yves
Walrand, Stéphane
4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia
title 4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia
title_full 4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia
title_fullStr 4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia
title_full_unstemmed 4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia
title_short 4E‐BP1 and 4E‐BP2 double knockout mice are protected from aging‐associated sarcopenia
title_sort 4e‐bp1 and 4e‐bp2 double knockout mice are protected from aging‐associated sarcopenia
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6596930/
https://www.ncbi.nlm.nih.gov/pubmed/30927336
http://dx.doi.org/10.1002/jcsm.12412
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