| Literature DB >> 31211694 |
Alessia De Caneva1, Fabiola Porro1, Giulia Bortolussi1, Riccardo Sola1, Michela Lisjak1, Adi Barzel2, Mauro Giacca1, Mark A Kay3, Kristian Vlahoviček4, Lorena Zentilin1, Andrés F Muro1.
Abstract
Non-integrative AAV-mediated gene therapy in the liver is effective in adult patients, but faces limitations in pediatric settings due to episomal DNA loss during hepatocyte proliferation. Gene targeting is a promising approach by permanently modifying the genome. We previously rescued neonatal lethality in Crigler-Najjar mice by inserting a promoterless human uridine glucuronosyl transferase A1 (UGT1A1) cDNA in exon 14 of the albumin gene, without the use of nucleases. To increase recombination rate and therapeutic efficacy, here we used CRISPR/SaCas9. Neonatal mice were transduced with two AAVs: one expressing the SaCas9 and sgRNA, and one containing a promoterless cDNA flanked by albumin homology regions. Targeting efficiency increased ~26-fold with an eGFP reporter cDNA, reaching up to 24% of eGFP-positive hepatocytes. Next, we fully corrected the diseased phenotype of Crigler-Najjar mice by targeting the hUGT1A1 cDNA. Treated mice had normal plasma bilirubin up to 10 months after administration, hUGT1A1 protein levels were ~6-fold higher than in WT liver, with a 90-fold increase in recombination rate. Liver histology, inflammatory markers, and plasma albumin were normal in treated mice, with no off-targets in predicted sites. Thus, the improved efficacy and reassuring safety profile support the potential application of the proposed approach to other liver diseases.Entities:
Keywords: Gene therapy; Genetics; Hepatology; Monogenic diseases; Mouse models
Year: 2019 PMID: 31211694 PMCID: PMC6693827 DOI: 10.1172/jci.insight.128863
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708