Literature DB >> 7743920

Disruption of intermediate filament organization leads to structural defects at the intersomite junction in Xenopus myotomal muscle.

R B Cary1, M W Klymkowsky.   

Abstract

In mature striated muscle, intermediate filaments (IFs) are associated with the periphery of Z-discs and sites of myofibril-membrane attachment. Previously T. Schultheiss, Z. X. Lin, H. Ishikawa, I. Zamir, C. J. Stoeckert and H. Holtzer (1991) J. Cell Biol. 114, 953) reported that the disruption of IF organization in cultured chick myotubes had no detectable effect on muscle cell structure. Cultured muscle is not, however, under the mechanical loads characteristic of muscle in situ. The dorsal myotomal muscle (DMM) of the Xenopus tadpole provides an accessible model system in which to study the effects of mutant IF proteins on an intact, functional muscle. DNAs encoding truncated forms of Xenopus vimentin or desmin were injected into fertilized Xenopus eggs. Embryos were allowed to develop to the tadpole stage and then examined by confocal or electron microscopy. DMM cells containing the truncated IF polypeptides displayed disorganized IF systems. While the alignment of Z-lines appeared unaffected, cells accumulating mutant IF polypeptides displayed abnormal organization at the intersomite junction. Myocyte termini are normally characterized by deep invaginations of the sarcolemma. In myocytes expressing mutated IF polypeptides, these membrane invaginations were reduced or completely absent. Furthermore, the attachment of myofibrils to the junctional membrane was often aberrant or completely disrupted. These results suggest that in active muscle IFs play an important role in the organization and/or stabilization of myofibril-membrane attachment sites.

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Year:  1995        PMID: 7743920     DOI: 10.1242/dev.121.4.1041

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  9 in total

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Review 2.  Intermediate filaments as dynamic structures.

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5.  Chibby functions in Xenopus ciliary assembly, embryonic development, and the regulation of gene expression.

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6.  Desmin is essential for the tensile strength and integrity of myofibrils but not for myogenic commitment, differentiation, and fusion of skeletal muscle.

Authors:  Z Li; M Mericskay; O Agbulut; G Butler-Browne; L Carlsson; L E Thornell; C Babinet; D Paulin
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Review 7.  Filaments and phenotypes: cellular roles and orphan effects associated with mutations in cytoplasmic intermediate filament proteins.

Authors:  Michael W Klymkowsky
Journal:  F1000Res       Date:  2019-09-30

8.  Knockdown of desmin in zebrafish larvae affects interfilament spacing and mechanical properties of skeletal muscle.

Authors:  Mei Li; Monika Andersson-Lendahl; Thomas Sejersen; Anders Arner
Journal:  J Gen Physiol       Date:  2013-03       Impact factor: 4.086

9.  Disruption of muscle architecture and myocardial degeneration in mice lacking desmin.

Authors:  D J Milner; G Weitzer; D Tran; A Bradley; Y Capetanaki
Journal:  J Cell Biol       Date:  1996-09       Impact factor: 10.539

  9 in total

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