Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle

A null mutation was introduced into the mouse desmin gene by homologous recombination. The desmin knockout mice (Des −/−) develop normally and are fertile. However, defects were observed after birth in skeletal, smooth, and cardiac muscles (Li, Z., E. Colucci-Guyon, M. Pincon-Raymond, M. Mericskay,...

Descripción completa

Detalles Bibliográficos
Autores principales: Li, Zhenlin, Mericskay, Mathias, Agbulut, Onnik, Butler-Browne, Gillian, Carlsson, Lena, Thornell, Lars-Eric, Babinet, Charles, Paulin, Denise
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1997
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2139820/
https://www.ncbi.nlm.nih.gov/pubmed/9314534
_version_ 1782143885390118912
author Li, Zhenlin
Mericskay, Mathias
Agbulut, Onnik
Butler-Browne, Gillian
Carlsson, Lena
Thornell, Lars-Eric
Babinet, Charles
Paulin, Denise
author_facet Li, Zhenlin
Mericskay, Mathias
Agbulut, Onnik
Butler-Browne, Gillian
Carlsson, Lena
Thornell, Lars-Eric
Babinet, Charles
Paulin, Denise
author_sort Li, Zhenlin
collection PubMed
description A null mutation was introduced into the mouse desmin gene by homologous recombination. The desmin knockout mice (Des −/−) develop normally and are fertile. However, defects were observed after birth in skeletal, smooth, and cardiac muscles (Li, Z., E. Colucci-Guyon, M. Pincon-Raymond, M. Mericskay, S. Pournin, D. Paulin, and C. Babinet. 1996. Dev. Biol. 175:362–366; Milner, D.J., G. Weitzer, D. Tran, A. Bradley, and Y. Capetanaki. 1996. J. Cell Biol. 134:1255– 1270). In the present study we have carried out a detailed analysis of somitogenesis, muscle formation, maturation, degeneration, and regeneration in Des −/− mice. Our results demonstrate that all early stages of muscle differentiation and cell fusion occur normally. However, after birth, modifications were observed essentially in weight-bearing muscles such as the soleus or continually used muscles such as the diaphragm and the heart. In the absence of desmin, mice were weaker and fatigued more easily. The lack of desmin renders these fibers more susceptible to damage during contraction. We observed a process of degeneration of myofibers, accompanied by macrophage infiltration, and followed by a process of regeneration. These cycles of degeneration and regeneration resulted in a relative increase in slow myosin heavy chain (MHC) and decrease in fast MHC. Interestingly, this second wave of myofibrillogenesis during regeneration was often aberrant and showed signs of disorganization. Subsarcolemmal accumulation of mitochondria were also observed in these muscles. The lack of desmin was not compensated by an upregulation of vimentin in these mice either during development or regeneration. Absence of desmin filaments within the sarcomere does not interfere with primary muscle formation or regeneration. However, myofibrillogenesis in regenerating fibers is often abortive, indicating that desmin may be implicated in this repair process. The results presented here show that desmin is essential to maintain the structural integrity of highly solicited skeletal muscle.
format Text
id pubmed-2139820
institution National Center for Biotechnology Information
language English
publishDate 1997
publisher The Rockefeller University Press
record_format MEDLINE/PubMed
spelling pubmed-21398202008-05-01 Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle Li, Zhenlin Mericskay, Mathias Agbulut, Onnik Butler-Browne, Gillian Carlsson, Lena Thornell, Lars-Eric Babinet, Charles Paulin, Denise J Cell Biol Article A null mutation was introduced into the mouse desmin gene by homologous recombination. The desmin knockout mice (Des −/−) develop normally and are fertile. However, defects were observed after birth in skeletal, smooth, and cardiac muscles (Li, Z., E. Colucci-Guyon, M. Pincon-Raymond, M. Mericskay, S. Pournin, D. Paulin, and C. Babinet. 1996. Dev. Biol. 175:362–366; Milner, D.J., G. Weitzer, D. Tran, A. Bradley, and Y. Capetanaki. 1996. J. Cell Biol. 134:1255– 1270). In the present study we have carried out a detailed analysis of somitogenesis, muscle formation, maturation, degeneration, and regeneration in Des −/− mice. Our results demonstrate that all early stages of muscle differentiation and cell fusion occur normally. However, after birth, modifications were observed essentially in weight-bearing muscles such as the soleus or continually used muscles such as the diaphragm and the heart. In the absence of desmin, mice were weaker and fatigued more easily. The lack of desmin renders these fibers more susceptible to damage during contraction. We observed a process of degeneration of myofibers, accompanied by macrophage infiltration, and followed by a process of regeneration. These cycles of degeneration and regeneration resulted in a relative increase in slow myosin heavy chain (MHC) and decrease in fast MHC. Interestingly, this second wave of myofibrillogenesis during regeneration was often aberrant and showed signs of disorganization. Subsarcolemmal accumulation of mitochondria were also observed in these muscles. The lack of desmin was not compensated by an upregulation of vimentin in these mice either during development or regeneration. Absence of desmin filaments within the sarcomere does not interfere with primary muscle formation or regeneration. However, myofibrillogenesis in regenerating fibers is often abortive, indicating that desmin may be implicated in this repair process. The results presented here show that desmin is essential to maintain the structural integrity of highly solicited skeletal muscle. The Rockefeller University Press 1997-10-06 /pmc/articles/PMC2139820/ /pubmed/9314534 Text en This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Li, Zhenlin
Mericskay, Mathias
Agbulut, Onnik
Butler-Browne, Gillian
Carlsson, Lena
Thornell, Lars-Eric
Babinet, Charles
Paulin, Denise
Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle
title Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle
title_full Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle
title_fullStr Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle
title_full_unstemmed Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle
title_short Desmin Is Essential for the Tensile Strength and Integrity of Myofibrils but Not for Myogenic Commitment, Differentiation, and Fusion of Skeletal Muscle
title_sort desmin is essential for the tensile strength and integrity of myofibrils but not for myogenic commitment, differentiation, and fusion of skeletal muscle
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2139820/
https://www.ncbi.nlm.nih.gov/pubmed/9314534
work_keys_str_mv AT lizhenlin desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle
AT mericskaymathias desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle
AT agbulutonnik desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle
AT butlerbrownegillian desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle
AT carlssonlena desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle
AT thornelllarseric desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle
AT babinetcharles desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle
AT paulindenise desminisessentialforthetensilestrengthandintegrityofmyofibrilsbutnotformyogeniccommitmentdifferentiationandfusionofskeletalmuscle

Ejemplares similares