Impaired regeneration in LGMD2A supported by increased Pax7 positive satellite cell content and muscle specific microRNA dysregulation

dc.contributor.authorRosales, Xiomara Q.
dc.contributor.authorMalik, Vinod
dc.contributor.authorSneh, Amita
dc.contributor.authorChen, Lei
dc.contributor.authorLewis, Sarah
dc.contributor.authorKota, Janaiah
dc.contributor.authorGastier-Foster, Julie M.
dc.contributor.authorAstbury, Caroline
dc.contributor.authorPyatt, Rob
dc.contributor.authorReshmi, Shalini
dc.contributor.authorRodino-Klapac, Louise R.
dc.contributor.authorClark, K. Reed
dc.contributor.authorMendell, Jerry R.
dc.contributor.authorSahenk, Zarife
dc.date.accessioned2020-01-10T15:21:40Z
dc.date.available2020-01-10T15:21:40Z
dc.date.issued2013-05
dc.description.abstractIntroduction—Recent in vitro studies suggest that CAPN3 deficiency leads initially to accelerated myofiber formation followed by depletion of satellite cells (SC). In normal muscle, upregulation of miR-1 and miR-206 facilitates transition from proliferating SCs to differentiating myogenic progenitors. Methods—We examined the histopathological stages, Pax7 SC content, and muscle specific microRNA expression in biopsy specimens from well-characterized LGMD 2A patients to gain insight into disease pathogenesis. Results—Three distinct stages of pathological changes were identified that represented the continuum of the dystrophic process from prominent inflammation with necrosis and regeneration to prominent fibrosis, which correlated with age and disease duration. Pax7-positive SCs were highest in fibrotic group and correlated with down-regulation of miR-1, miR-133a, and miR-206. Conclusions—These observations, and other published reports, are consistent with microRNA dysregulation leading to inability of Pax7-positive SCs to transit from proliferation to differentiation. This results in impaired regeneration and fibrosis.en_US
dc.description.sponsorshipThis work was supported by NIH NIAMS U54 AR050733-05, Jesse’s Journey, and the muscular Dystrophy Associationen_US
dc.identifier.doi10.1002/mus.23669
dc.identifier.urihttps://hdl.handle.net/1805/21814
dc.publisherMuscle & Nerveen_US
dc.subjectLGMD2Aen_US
dc.subjectFibrosisen_US
dc.subjectmicroRNAen_US
dc.subjectmuscle regenerationen_US
dc.titleImpaired regeneration in LGMD2A supported by increased Pax7 positive satellite cell content and muscle specific microRNA dysregulationen_US
dc.typeArticleen_US
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