Literature DB >> 12037582

Localization of alpha 7 integrins and dystrophin suggests potential for both lateral and longitudinal transmission of tension in large mammalian muscles.

Angelika C Paul1, Philip W Sheard, Stephen J Kaufman, Marilyn J Duxson.   

Abstract

Non-primate mammalian muscles with fascicles above 35 mm in length are composed predominantly of arrays of short, non-spanning muscle fibres, which terminate within the belly of the muscle fascicle at one or both ends. We have previously described the morphological form of various muscle-to-muscle and muscle-to-matrix junctions which are likely involved in tension transmission within one such muscle - the guinea pig sternomastoid muscle (Young et al. 2000). Here, we use immunohistochemistry to investigate the cell adhesion molecules present at these junctions. We find strong immunoreactivity against the alpha 7B integrin subunit and dystrophin, and slight reactivity against the alpha 7A integrin at all intrafascicular fibre terminations (IFTs), as well as at the muscle-tendon junction (MTJ). Tenascin, the sole ligand for alpha 9 beta 1 integrin, was absent from IFTs but present at the MTJ, suggesting the two sites are molecularly distinct. In addition to their expression at junctional sites, alpha 7B integrin and dystrophin were also expressed ubiquitously along the non-junctional sarcolemma, suggesting potential involvement in diffuse lateral transmission of tension between adjacent fibres. We conclude that the distribution of alpha 7 beta 1 integrins and dystrophin in series-fibred muscles suggests they are involved in transmission of tension from intrafascicularly terminating fibres to neighbouring fibres lying both in-series and in-parallel, via the extracellular matrix (ECM).

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Year:  2002        PMID: 12037582     DOI: 10.1007/s00441-002-0526-y

Source DB:  PubMed          Journal:  Cell Tissue Res        ISSN: 0302-766X            Impact factor:   5.249


  18 in total

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4.  Dilated cardiomyopathy mutations in δ-sarcoglycan exert a dominant-negative effect on cardiac myocyte mechanical stability.

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5.  Activation of AKT signaling promotes cell growth and survival in α7β1 integrin-mediated alleviation of muscular dystrophy.

Authors:  Marni D Boppart; Dean J Burkin; Stephen J Kaufman
Journal:  Biochim Biophys Acta       Date:  2011-01-07

6.  Transgenic expression of {alpha}7{beta}1 integrin maintains muscle integrity, increases regenerative capacity, promotes hypertrophy, and reduces cardiomyopathy in dystrophic mice.

Authors:  Dean J Burkin; Gregory Q Wallace; Derek J Milner; Eric J Chaney; James A Mulligan; Stephen J Kaufman
Journal:  Am J Pathol       Date:  2005-01       Impact factor: 4.307

7.  Localization and function of Xinα in mouse skeletal muscle.

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Journal:  Am J Physiol Cell Physiol       Date:  2013-03-13       Impact factor: 4.249

Review 8.  Tissue engineering of functional skeletal muscle: challenges and recent advances.

Authors:  Weining Bian; Nenad Bursac
Journal:  IEEE Eng Med Biol Mag       Date:  2008 Sep-Oct

Review 9.  Physiology and metabolism of tissue-engineered skeletal muscle.

Authors:  Cindy S Cheng; Brittany N J Davis; Lauran Madden; Nenad Bursac; George A Truskey
Journal:  Exp Biol Med (Maywood)       Date:  2014-06-09

Review 10.  Design, evaluation, and application of engineered skeletal muscle.

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Journal:  Methods       Date:  2015-10-06       Impact factor: 3.608

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