A humanized mouse model for adeno-associated viral gene therapy

Author:

Barzi Mercedes,Chen Tong,Gonzalez Trevor J.,Pankowicz Francis P.,Oh Seh Hoon,Streff Helen L.ORCID,Rosales AlanORCID,Ma Yunhan,Collias Sabrina,Woodfield Sarah E.,Diehl Anna MaeORCID,Vasudevan Sanjeev A.,Galvan Thao N.ORCID,Goss John,Gersbach Charles A.ORCID,Bissig-Choisat Beatrice,Asokan AravindORCID,Bissig Karl-DimiterORCID

Abstract

AbstractClinical translation of AAV-mediated gene therapy requires preclinical development across different experimental models, often confounded by variable transduction efficiency. Here, we describe a human liver chimeric transgene-free Il2rg−/−/Rag2−/−/Fah−/−/Aavr−/− (TIRFA) mouse model overcoming this translational roadblock, by combining liver humanization with AAV receptor (AAVR) ablation, rendering murine cells impermissive to AAV transduction. Using human liver chimeric TIRFA mice, we demonstrate increased transduction of clinically used AAV serotypes in primary human hepatocytes compared to humanized mice with wild-type AAVR. Further, we demonstrate AAV transduction in human teratoma-derived primary cells and liver cancer tissue, displaying the versatility of the humanized TIRFA mouse. From a mechanistic perspective, our results support the notion that AAVR functions as both an entry receptor and an intracellular receptor essential for transduction. The TIRFA mouse should allow prediction of AAV gene transfer efficiency and the study of AAV vector biology in a preclinical human setting.

Funder

U.S. Department of Health & Human Services | NIH | National Institute of Diabetes and Digestive and Kidney Diseases

Avachrome Incorporation

Publisher

Springer Science and Business Media LLC

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