Differential regulation of myofibrillar proteins in skeletal muscles of septic mice

Differential regulation of myofibrillar proteins in skeletal muscles of septic mice

Abstract Sepsis elicits skeletal muscle atrophy as a result of decreased total protein synthesis and/or increased total protein degradation. It is unknown how and whether sepsis differentially affects the expression of specific myofibrillar proteins in respiratory and limb muscles. In this study, we...

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Main Authors: Vanessa Moarbes, Dominique Mayaki, Laurent Huck, Philippe Leblanc, Theodoros Vassilakopoulos, Basil J. Petrof, Sabah N. A. Hussain
Format: Article
Language:English
Published: Wiley 2019-10-01
Series:Physiological Reports
Subjects:
sepsis
muscle atrophy
proteasome
autophagy
myofibrillar proteins
myosin
Online Access:https://doi.org/10.14814/phy2.14248
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spelling doaj-c1a6190db40244c5a5fd5408c913dbe52020-11-25T03:08:09ZengWileyPhysiological Reports2051-817X2019-10-01720n/an/a10.14814/phy2.14248Differential regulation of myofibrillar proteins in skeletal muscles of septic miceVanessa Moarbes0Dominique Mayaki1Laurent Huck2Philippe Leblanc3Theodoros Vassilakopoulos4Basil J. Petrof5Sabah N. A. Hussain6Meakins‐Christie Laboratories and Translational Research in Respiratory Diseases Program Research Institute of the McGill University Health Centre Montréal Québec CanadaMeakins‐Christie Laboratories and Translational Research in Respiratory Diseases Program Research Institute of the McGill University Health Centre Montréal Québec CanadaMeakins‐Christie Laboratories and Translational Research in Respiratory Diseases Program Research Institute of the McGill University Health Centre Montréal Québec CanadaMeakins‐Christie Laboratories and Translational Research in Respiratory Diseases Program Research Institute of the McGill University Health Centre Montréal Québec CanadaCritical Care Department, National & Kapodistrian University of Athens, Medical School, Evgenideion Hospital Athens GreeceMeakins‐Christie Laboratories and Translational Research in Respiratory Diseases Program Research Institute of the McGill University Health Centre Montréal Québec CanadaMeakins‐Christie Laboratories and Translational Research in Respiratory Diseases Program Research Institute of the McGill University Health Centre Montréal Québec CanadaAbstract Sepsis elicits skeletal muscle atrophy as a result of decreased total protein synthesis and/or increased total protein degradation. It is unknown how and whether sepsis differentially affects the expression of specific myofibrillar proteins in respiratory and limb muscles. In this study, we measured the effects of sepsis myofibrillar mRNAs and their corresponding protein levels in the diaphragm (DIA) and tibialis anterior (TA) muscles in a murine cecal ligation and perforation (CLP) model of sepsis. Male mice (C57/BL6j) underwent CLP‐induced sepsis. Sham‐operated mice were subjected to the same surgical procedures, except for CLP. Mice were euthanized 24, 48, or 96 h postsurgery. Transcript and protein levels of autophagy‐related genes, ubiquitin E3 ligases, and several myofibrillar genes were quantified. Sepsis elicited transient fiber atrophy in the DIA and prolonged atrophy in the TA. Atrophy was coincident with increased autophagy and ubiquitin E3 ligase expression. Myosin heavy chain isoforms decreased at 24 h in the DIA and across the time‐course in the TA, myosin light chain isoforms decreased across the time‐course in both muscles, and troponins T and C as well as tropomyosin decreased after 24 and 48 h in both the DIA and TA. α‐Actin and troponin I were unaffected by sepsis. Sepsis‐induced decreases in myofibrillar protein levels coincided with decreased mRNA expressions of these proteins, suggesting that transcriptional inhibition is involved. We hypothesize that sepsis‐induced muscle atrophy is mediated by decreased transcription and enhanced degradation of specific myofibrillar proteins, including myosin heavy and light chains, troponin C, troponin T, and tropomyosin.https://doi.org/10.14814/phy2.14248sepsismuscle atrophyproteasomeautophagymyofibrillar proteinsmyosin
collection DOAJ
language English
format Article
sources DOAJ
author Vanessa Moarbes
Dominique Mayaki
Laurent Huck
Philippe Leblanc
Theodoros Vassilakopoulos
Basil J. Petrof
Sabah N. A. Hussain
spellingShingle Vanessa Moarbes
Dominique Mayaki
Laurent Huck
Philippe Leblanc
Theodoros Vassilakopoulos
Basil J. Petrof
Sabah N. A. Hussain
Differential regulation of myofibrillar proteins in skeletal muscles of septic mice
Physiological Reports
sepsis
muscle atrophy
proteasome
autophagy
myofibrillar proteins
myosin
author_facet Vanessa Moarbes
Dominique Mayaki
Laurent Huck
Philippe Leblanc
Theodoros Vassilakopoulos
Basil J. Petrof
Sabah N. A. Hussain
author_sort Vanessa Moarbes
title Differential regulation of myofibrillar proteins in skeletal muscles of septic mice
title_short Differential regulation of myofibrillar proteins in skeletal muscles of septic mice
title_full Differential regulation of myofibrillar proteins in skeletal muscles of septic mice
title_fullStr Differential regulation of myofibrillar proteins in skeletal muscles of septic mice
title_full_unstemmed Differential regulation of myofibrillar proteins in skeletal muscles of septic mice
title_sort differential regulation of myofibrillar proteins in skeletal muscles of septic mice
publisher Wiley
series Physiological Reports
issn 2051-817X
publishDate 2019-10-01
description Abstract Sepsis elicits skeletal muscle atrophy as a result of decreased total protein synthesis and/or increased total protein degradation. It is unknown how and whether sepsis differentially affects the expression of specific myofibrillar proteins in respiratory and limb muscles. In this study, we measured the effects of sepsis myofibrillar mRNAs and their corresponding protein levels in the diaphragm (DIA) and tibialis anterior (TA) muscles in a murine cecal ligation and perforation (CLP) model of sepsis. Male mice (C57/BL6j) underwent CLP‐induced sepsis. Sham‐operated mice were subjected to the same surgical procedures, except for CLP. Mice were euthanized 24, 48, or 96 h postsurgery. Transcript and protein levels of autophagy‐related genes, ubiquitin E3 ligases, and several myofibrillar genes were quantified. Sepsis elicited transient fiber atrophy in the DIA and prolonged atrophy in the TA. Atrophy was coincident with increased autophagy and ubiquitin E3 ligase expression. Myosin heavy chain isoforms decreased at 24 h in the DIA and across the time‐course in the TA, myosin light chain isoforms decreased across the time‐course in both muscles, and troponins T and C as well as tropomyosin decreased after 24 and 48 h in both the DIA and TA. α‐Actin and troponin I were unaffected by sepsis. Sepsis‐induced decreases in myofibrillar protein levels coincided with decreased mRNA expressions of these proteins, suggesting that transcriptional inhibition is involved. We hypothesize that sepsis‐induced muscle atrophy is mediated by decreased transcription and enhanced degradation of specific myofibrillar proteins, including myosin heavy and light chains, troponin C, troponin T, and tropomyosin.
topic sepsis
muscle atrophy
proteasome
autophagy
myofibrillar proteins
myosin
url https://doi.org/10.14814/phy2.14248
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