α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration

α1-Syntrophin is a member of the family of dystrophin-associated proteins; it has been shown to recruit neuronal nitric oxide synthase and the water channel aquaporin-4 to the sarcolemma by its PSD-95/SAP-90, Discs-large, ZO-1 homologous domain. To examine the role of α1-syntrophin in muscle regener...

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Autores principales: Hosaka, Yukio, Yokota, Toshifumi, Miyagoe-Suzuki, Yuko, Yuasa, Katsutoshi, Imamura, Michihiro, Matsuda, Ryoichi, Ikemoto, Takaaki, Kameya, Shuhei, Takeda, Shin'ichi
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2002
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2173222/
https://www.ncbi.nlm.nih.gov/pubmed/12221071
http://dx.doi.org/10.1083/jcb.200204076
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author Hosaka, Yukio
Yokota, Toshifumi
Miyagoe-Suzuki, Yuko
Yuasa, Katsutoshi
Imamura, Michihiro
Matsuda, Ryoichi
Ikemoto, Takaaki
Kameya, Shuhei
Takeda, Shin'ichi
author_facet Hosaka, Yukio
Yokota, Toshifumi
Miyagoe-Suzuki, Yuko
Yuasa, Katsutoshi
Imamura, Michihiro
Matsuda, Ryoichi
Ikemoto, Takaaki
Kameya, Shuhei
Takeda, Shin'ichi
author_sort Hosaka, Yukio
collection PubMed
description α1-Syntrophin is a member of the family of dystrophin-associated proteins; it has been shown to recruit neuronal nitric oxide synthase and the water channel aquaporin-4 to the sarcolemma by its PSD-95/SAP-90, Discs-large, ZO-1 homologous domain. To examine the role of α1-syntrophin in muscle regeneration, we injected cardiotoxin into the tibialis anterior muscles of α1-syntrophin–null (α1syn(−/−)) mice. After the treatment, α1syn(−/−) muscles displayed remarkable hypertrophy and extensive fiber splitting compared with wild-type regenerating muscles, although the untreated muscles of the mutant mice showed no gross histological change. In the hypertrophied muscles of the mutant mice, the level of insulin-like growth factor-1 transcripts was highly elevated. Interestingly, in an early stage of the regeneration process, α1syn(−/−) mice showed remarkably deranged neuromuscular junctions (NMJs), accompanied by impaired ability to exercise. The contractile forces were reduced in α1syn(−/−) regenerating muscles. Our results suggest that the lack of α1-syntrophin might be responsible in part for the muscle hypertrophy, abnormal synapse formation at NMJs, and reduced force generation during regeneration of dystrophin-deficient muscle, all of which are typically observed in the early stages of Duchenne muscular dystrophy patients.
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spelling pubmed-21732222008-05-01 α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration Hosaka, Yukio Yokota, Toshifumi Miyagoe-Suzuki, Yuko Yuasa, Katsutoshi Imamura, Michihiro Matsuda, Ryoichi Ikemoto, Takaaki Kameya, Shuhei Takeda, Shin'ichi J Cell Biol Article α1-Syntrophin is a member of the family of dystrophin-associated proteins; it has been shown to recruit neuronal nitric oxide synthase and the water channel aquaporin-4 to the sarcolemma by its PSD-95/SAP-90, Discs-large, ZO-1 homologous domain. To examine the role of α1-syntrophin in muscle regeneration, we injected cardiotoxin into the tibialis anterior muscles of α1-syntrophin–null (α1syn(−/−)) mice. After the treatment, α1syn(−/−) muscles displayed remarkable hypertrophy and extensive fiber splitting compared with wild-type regenerating muscles, although the untreated muscles of the mutant mice showed no gross histological change. In the hypertrophied muscles of the mutant mice, the level of insulin-like growth factor-1 transcripts was highly elevated. Interestingly, in an early stage of the regeneration process, α1syn(−/−) mice showed remarkably deranged neuromuscular junctions (NMJs), accompanied by impaired ability to exercise. The contractile forces were reduced in α1syn(−/−) regenerating muscles. Our results suggest that the lack of α1-syntrophin might be responsible in part for the muscle hypertrophy, abnormal synapse formation at NMJs, and reduced force generation during regeneration of dystrophin-deficient muscle, all of which are typically observed in the early stages of Duchenne muscular dystrophy patients. The Rockefeller University Press 2002-09-16 /pmc/articles/PMC2173222/ /pubmed/12221071 http://dx.doi.org/10.1083/jcb.200204076 Text en Copyright © 2002, The Rockefeller University Press 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
Hosaka, Yukio
Yokota, Toshifumi
Miyagoe-Suzuki, Yuko
Yuasa, Katsutoshi
Imamura, Michihiro
Matsuda, Ryoichi
Ikemoto, Takaaki
Kameya, Shuhei
Takeda, Shin'ichi
α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration
title α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration
title_full α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration
title_fullStr α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration
title_full_unstemmed α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration
title_short α1-Syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration
title_sort α1-syntrophin–deficient skeletal muscle exhibits hypertrophy and aberrant formation of neuromuscular junctions during regeneration
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2173222/
https://www.ncbi.nlm.nih.gov/pubmed/12221071
http://dx.doi.org/10.1083/jcb.200204076
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