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Gene therapy for progressive familial intrahepatic cholestasis type 3 in a clinically relevant mouse model

Nat Commun.. 2019; 
Weber ND1, Odriozola L2, Martínez-García J2, Ferrer V3, Douar A3, Bénichou B3, González-Aseguinolaza G4,5,6, Smerdou C7,8.
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Gene Synthesis Synthetic wildtype and codonoptimized sequences of human ABCB4 cDNA coding for MDR3 isoforms A (NCBI Reference Sequence: NP_000434.1), B (NP_061337.1), and C (NP_061338.1) were obtained from GenScript (Nanjing, China) cloned into pUC57 flanked by SalI and NdeI sites (pU57-MDR3). Get A Quote

摘要

Progressive familial intrahepatic cholestasis type 3 (PFIC3) is a rare monogenic disease caused by mutations in the ABCB4 gene, resulting in a reduction in biliary phosphatidylcholine. Reduced biliary phosphatidylcholine cannot counteract the detergent effects of bile salts, leading to cholestasis, cholangitis, cirrhosis and ultimately liver failure. Here, we report results from treating two- or five-week-old Abcb4-/- mice with an AAV vector expressing human ABCB4, resulting in significant decreases of PFIC3 disease biomarkers. All male mice achieved a sustained therapeutic effect up through 12 weeks, but the effect was achieved in only 50% of females. However, two-week-old females receiving a second inoculatio... More

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