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Systemic AAV-Mediated β-Sarcoglycan Delivery Targeting Cardiac and Skeletal Muscle Ameliorates Histological and Functional Deficits in LGMD2E Mice.

Mol. Ther.. 2017; 
PozsgaiEric R,GriffinDanielle A,HellerKristin N,MendellJerry R,Rodino-KlapacLoui
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Codon Optimization Thefull-lengthhumanb-sarcoglycancDNA(GenBank:NM_0034994. 3)wascodon-optimizedandsynthesizedbyGenScript. Get A Quote

摘要

Limb-girdle muscular dystrophy type 2E (LGMD2E), resulting from mutations in β-sarcoglycan (SGCB), is a progressive dystrophy with deteriorating muscle function, respiratory failure, and cardiomyopathy in 50% or more of LGMD2E patients. SGCB knockout mice share many of the phenotypic deficiencies of LGMD2E patients. To investigate systemic SGCB gene transfer to treat skeletal and cardiac muscle deficits, we designed a self-complementary AAVrh74 vector containing a codon-optimized human SGCB transgene driven by a muscle-specific promoter. We delivered scAAV.MHCK7.hSGCB through the tail vein of SGCB mice to provide a rationale for a clinical trial that would lead to clinically meaningful results. Th... More

关键词

AAV,LGMD2E,gene therapy,limb-girdle muscular dystrophy,muscular dystrophy,β-sarcogl