Literature DB >> 12045834

Impaired regeneration of dystrophin-deficient muscle fibers is caused by exhaustion of myogenic cells.

M A M Luz1, M J Marques, H Santo Neto.   

Abstract

Duchenne muscular dystrophy is one of the most devastating myopathies. Muscle fibers undergo necrosis and lose their ability to regenerate, and this may be related to increased interstitial fibrosis or the exhaustion of satellite cells. In this study, we used mdx mice, an animal model of Duchenne muscular dystrophy, to assess whether muscle fibers lose their ability to regenerate after repeated cycles of degeneration-regeneration and to establish the role of interstitial fibrosis or exhaustion of satellite cells in this process. Repeated degenerative-regenerative cycles were induced by the injection of bupivacaine (33 mg/kg), a myotoxic agent. Bupivacaine was injected weekly into the right tibialis anterior muscle of male, 8-week-old mdx (N = 20) and C57Bl/10 (control, N = 10) mice for 20 and 50 weeks. Three weeks after the last injection, the mice were killed and the proportion of regenerated fibers was counted and reported as a fibrosis index. Twenty weekly bupivacaine injections did not change the ability of mdx muscle to regenerate. However, after 50 weekly bupivacaine injections, there was a significant decrease in the regenerative response. There was no correlation between the inability to regenerate and the increase in interstitial fibrosis. These results show that after prolonged repeated cycles of degeneration-regeneration, mdx muscle loses its ability to regenerate because of the exhaustion of satellite cells, rather than because of an increase in interstitial fibrosis. This finding may be relevant to cell and gene therapy in the treatment of Duchenne muscular dystrophy.

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Year:  2002        PMID: 12045834     DOI: 10.1590/s0100-879x2002000600009

Source DB:  PubMed          Journal:  Braz J Med Biol Res        ISSN: 0100-879X            Impact factor:   2.590


  32 in total

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2.  Changes in calsequestrin, TNF-α, TGF-β and MyoD levels during the progression of skeletal muscle dystrophy in mdx mice: a comparative analysis of the quadriceps, diaphragm and intrinsic laryngeal muscles.

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4.  Photobiomodulation therapy protects skeletal muscle and improves muscular function of mdx mice in a dose-dependent manner through modulation of dystrophin.

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5.  Genetic background affects properties of satellite cells and mdx phenotypes.

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Review 6.  Molecular circuitry of stem cell fate in skeletal muscle regeneration, ageing and disease.

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7.  Regulation of IRS1/Akt insulin signaling by microRNA-128a during myogenesis.

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8.  Highly efficient, functional engraftment of skeletal muscle stem cells in dystrophic muscles.

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9.  Impaired regeneration in LGMD2A supported by increased PAX7-positive satellite cell content and muscle-specific microrna dysregulation.

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10.  Nestin expression in end-stage disease in dystrophin-deficient heart: implications for regeneration from endogenous cardiac stem cells.

Authors:  Suzanne E Berry; Peter Andruszkiewicz; Ju Lan Chun; Jun Hong
Journal:  Stem Cells Transl Med       Date:  2013-09-25       Impact factor: 6.940

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