AAV2-mediated gene therapy for Bietti crystalline dystrophy provides functional CYP4V2 in multiple relevant cell models

Wang, J-H; Lidgerwood, GE; Daniszewski, M; Hu, ML; Roberts, GE; Wong, RCB; Hung, SSC; McClements, ME; Hewitt, AW; Pébay, A; Hickey, DG; Edwards, TL

Journal article

AAV2-mediated gene therapy for Bietti crystalline dystrophy provides functional CYP4V2 in multiple relevant cell models

Abstract:: Bietti crystalline dystrophy (BCD) is an inherited retinal disease (IRD) caused by mutations in the CYP4V2 gene. It is a relatively common cause of IRD in east Asia. A number of features of this disease make it highly amenable to gene supplementation therapy. This study aims to validate a series of essential precursor in vitro experiments prior to developing a clinical gene therapy for BCD. We demonstrated that HEK293, ARPE19, and patient induced pluripotent stem cell (iPSC)-derived RPE cells transduced with AAV2 vectors encoding codon optimization of CYP4V2 (AAV2.coCYP4V2) resulted in elevated protein expression levels of CYP4V2 compared to those transduced with AAV2 vectors encoding wild type CYP4V2 (AAV2.wtCYP4V2), as assessed by immunocytochemistry and western blot. Similarly, we observed significantly increased CYP4V2 enzyme activity in cells transduced with AAV2.coCYP4V2 compared to those transduced with AAV2.wtCYP4V2. We also showed CYP4V2 expression in human RPE/choroid explants transduced with AAV2.coCYP4V2 compared to those transduced with AAV2.wtCYP4V2. These preclinical data support the further development of a gene supplementation therapy for a currently untreatable blinding condition-BCD. Codon-optimized CYP4V2 transgene was superior to wild type in terms of protein expression and enzyme activity. Ex vivo culture of human RPE cells provided an effective approach to test AAV-mediated transgene delivery.

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Peer review status:: Peer reviewed

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APA Style

Wang, J.-H., Lidgerwood, G. E., Daniszewski, M., Hu, M. L., Roberts, G. E., Wong, R. C. B., Hung, S. S. C., McClements, M. E., Hewitt, A. W., Pébay, A., Hickey, D. G., & Edwards, T. L. (2022). AAV2-mediated gene therapy for Bietti crystalline dystrophy provides functional CYP4V2 in multiple relevant cell models. Scientific Reports, 12(1), 9525–9525.

MLA Style

Wang, J-H, et al. “AAV2-Mediated Gene Therapy for Bietti Crystalline Dystrophy Provides Functional CYP4V2 in Multiple Relevant Cell Models.” Scientific Reports, vol. 12, no. 1, 2022, pp. 9525–25.

Chicago Style

Wang, J-H, GE Lidgerwood, M Daniszewski, et al. 2022. “AAV2-Mediated Gene Therapy for Bietti Crystalline Dystrophy Provides Functional CYP4V2 in Multiple Relevant Cell Models.” Scientific Reports 12 (1): 9525–25.
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Files:: Wang_et_al_2022_AAV2-mediated_gene_therapy.pdf

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Publisher copy:: 10.1038/s41598-022-12210-8

Authors

+ Wang, J-H More by this author

Role:: Author

+ Lidgerwood, GE More by this author

Role:: Author
ORCID:: 0000-0002-1774-5944

+ Daniszewski, M More by this author

Role:: Author
ORCID:: 0000-0003-3468-4941

+ Hu, ML More by this author

Role:: Author
ORCID:: 0000-0003-3224-1434

+ Roberts, GE More by this author

Role:: Author

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+ NHMRC Senior Research Fellowship More from this funder

Grant:: 1153498

+ DHB Foundation More from this funder

+ Hector Maclean Scholarship More from this funder

+ the University of Melbourne Annemarie Mankiewicz-Zelkin Fellowship More from this funder

Publisher:: Nature Research
Journal:: Scientific Reports More from this journal
Volume:: 12
Issue:: 1
Pages:: 9525-9525
Article number:: 9525
Publication date:: 2022-06-09
DOI:: 10.1038/s41598-022-12210-8
EISSN:: 2045-2322
ISSN:: 2045-2322

Language:: English
Keywords:: Medicine

Pathology

Gene

Genetics

Biology

Bioinformatics

Dystrophy

Genetic enhancement
Pubs id:: 1263334
Local pid:: pubs:1263334
Source identifiers:: W4282923198
Deposit date:: 2026-04-24
ARK identifier:: ark:/29072/ora_26866f53cf3e466e84c5adc32447d7a2

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Licence:: CC Attribution (CC BY)

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AAV2-mediated gene therapy for Bietti crystalline dystrophy provides functional CYP4V2 in multiple relevant cell models

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