| Literature DB >> 23721401 |
François Monjaret1, Laurence Suel-Petat, Nathalie Bourg-Alibert, Anna Vihola, Sylvie Marchand, Carinne Roudaut, Evelyne Gicquel, Bjarne Udd, Isabelle Richard, Karine Charton.
Abstract
Mutations in dysferlin and anoctamin 5 are the cause of muscular disorders, with the main presentations as limb-girdle muscular dystrophy or Miyoshi type of distal myopathy. Both these proteins have been implicated in sarcolemmal resealing. On the basis of similarities in associated phenotypes and protein functions, we tested the hypothesis that ANO5 protein could compensate for dysferlin absence. We first defined that the main transcript of ANO5 expressed in skeletal muscle is the 22-exon full-length isoform, and we demonstrated that dysferlin-deficient (Dysf (prmd)) mice have lower Ano5 expression levels, an observation that further enhanced the rational of the tested hypothesis. We then showed that AAV-mediated transfer of human ANO5 (hANO5) did not lead to apparent toxicity in wild-type mice. Finally, we demonstrated that AAV-hANO5 injection was not able to compensate for dysferlin deficiency in the Dysf (prmd) mouse model or improve the membrane repair defect seen in the absence of dysferlin. Consequently, overexpressing hANO5 does not seem to provide a valuable therapeutic strategy for dysferlin deficiency.Entities:
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Year: 2013 PMID: 23721401 DOI: 10.1089/humc.2012.217
Source DB: PubMed Journal: Hum Gene Ther Clin Dev ISSN: 2324-8637 Impact factor: 5.032