AAV capsid bioengineering in primary human retina

Author:

Westhaus Adrian1,Eamegdool Steven S.2,Fernando Milan1,Fuller-Carter Paula3,Brunet Alicia A3,Rashwan Rabab3,Knight Maddison1,Daniszewski Maciej4,Lidgerwood Grace E.4,Pébay Alice4,Hewitt Alex5,Santilli Giorgia6,Thrasher Adrian J.6,Carvalho Livia S3,Gonzalez-Cordero Anai7,Jamieson Robyn V2,Lisowski Leszek1

Affiliation:

1. Children’s Medical Research Institute

2. Children's Medical Research Institute and Sydney Children’s Hospitals Network

3. The University of Western Australia

4. The University of Melbourne

5. University of Tasmania

6. University College London

7. The University of Sydney

Abstract

Abstract Adeno-associated viral (AAV) vector-mediated retinal gene therapy is an active field of both pre-clinical as well as clinical research. As with other gene therapy clinical targets, novel bioengineered AAV variants developed by directed evolution or rational design to possess unique desirable properties, are entering retinal gene therapy translational programs. However, it is becoming increasingly evident that predictive preclinical models are required to develop and functionally validate these novel AAVs prior to clinical studies. To this end, this study performed a large high-throughput screen of 51 existing AAV capsids in primary human retina explants and other models of the human retina. Furthermore, we applied transgene expression-based directed evolution to develop novel capsids for more efficient transduction of primary human retina cells and compared the top variants to the strongest existing benchmarks identified in the screening described above. A direct side-by-side comparison of the newly developed capsids in four different in vitro and ex vivo model systems of the human retina allowed us to identify novel AAV variants capable of high transgene expression in primary human retina cells.

Publisher

Research Square Platform LLC

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