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Systemic delivery of full-length dystrophin in Duchenne muscular dystrophy mice

Medicine and Health

Systemic delivery of full-length dystrophin in Duchenne muscular dystrophy mice

Y. Zhou, C. Zhang, et al.

Exciting advancements in gene therapy for Duchenne muscular dystrophy (DMD) are here! Researchers developed a triple vector system that effectively delivers full-length dystrophin, restoring crucial muscle function in *mdx* mice. This innovative approach, spearheaded by authors Yuan Zhou, Chen Zhang, Weidong Xiao, Roland W. Herzog, and Renzhi Han, shows promise for a mutation-independent treatment option.... show more
Abstract
Current gene therapy for Duchenne muscular dystrophy (DMD) utilizes adeno-associated virus (AAV) to deliver micro-dystrophin (µDys), which does not provide full protection for striated muscles as it lacks many important functional domains of full-length (FL) dystrophin. Here we develop a triple vector system to deliver FL-dystrophin into skeletal and cardiac muscles. We split FL-dystrophin into three fragments linked to two orthogonal pairs of split intein, allowing efficient assembly of FL-dystrophin. The three fragments packaged in myotropic AAV (MyoAAV4A) restore FL-dystrophin expression in both skeletal and cardiac muscles in male mdx mice. Dystrophin-glycoprotein complex components are also restored at the sarcolemma of dystrophic muscles. MyoAAV4A-delivered FL-dystrophin significantly improves muscle histopathology, contractility, and overall strength comparable to µDys, but unlike µDys, it also restores defective cavin 4 localization and associated signaling in mdx heart. Therefore, our data support the feasibility of a mutation-independent FL-dystrophin gene therapy for DMD, warranting further clinical development.
Publisher
Nature Communications
Published On
Jul 21, 2024
Authors
Yuan Zhou, Chen Zhang, Weidong Xiao, Roland W. Herzog, Renzhi Han
Tags
Duchenne muscular dystrophy
gene therapy
full-length dystrophin
adeno-associated virus
muscle restoration
mdx mice
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