Cross-species evolution of a highly potent AAV variant for therapeutic gene transfer and genome editing

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作者
Trevor J. Gonzalez
Katherine E. Simon
Leo O. Blondel
Marco M. Fanous
Angela L. Roger
Maribel Santiago Maysonet
Garth W. Devlin
Timothy J. Smith
Daniel K. Oh
L. Patrick Havlik
Ruth M. Castellanos Rivera
Jorge A. Piedrahita
Mai K. ElMallah
Charles A. Gersbach
Aravind Asokan
机构
[1] Duke University School of Medicine,Department of Molecular Genetics and Microbiology
[2] Duke University School of Medicine,Department of Surgery
[3] North Carolina State University College of Veterinary Medicine,Department of Pediatrics
[4] Duke University School of Medicine,StrideBio Inc.
[5] Research Triangle Park,Duke Regeneration Center
[6] Duke University School of Medicine,Department of Biomedical Engineering
[7] Duke University,undefined
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Recombinant adeno-associated viral (AAV) vectors are a promising gene delivery platform, but ongoing clinical trials continue to highlight a relatively narrow therapeutic window. Effective clinical translation is confounded, at least in part, by differences in AAV biology across animal species. Here, we tackle this challenge by sequentially evolving AAV capsid libraries in mice, pigs and macaques. We discover a highly potent, cross-species compatible variant (AAV.cc47) that shows improved attributes benchmarked against AAV serotype 9 as evidenced by robust reporter and therapeutic gene expression, Cre recombination and CRISPR genome editing in normal and diseased mouse models. Enhanced transduction efficiency of AAV.cc47 vectors is further corroborated in macaques and pigs, providing a strong rationale for potential clinical translation into human gene therapies. We envision that ccAAV vectors may not only improve predictive modeling in preclinical studies, but also clinical translatability by broadening the therapeutic window of AAV based gene therapies.
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