In vivo lentiviral vector gene therapy to cure hereditary tyrosinemia type 1 and prevent development of precancerous and cancerous lesions.
Clara T NicolasCaitlin J VanLithRaymond D HickeyZeji DuLori G HillinRebekah M GuthmanWilliam J CaoBenjamin HaugoAnnika LillegardDiya RoyAditya BhagwateDaniel O'BrienJean-Pierre A KocherRobert A KaiserStephen J RussellJoseph B LillegardPublished in: Nature communications (2022)
Conventional therapy for hereditary tyrosinemia type-1 (HT1) with 2-(2-nitro-4-trifluoromethylbenzoyl)-1,3-cyclohexanedione (NTBC) delays and in some cases fails to prevent disease progression to liver fibrosis, liver failure, and activation of tumorigenic pathways. Here we demonstrate cure of HT1 by direct, in vivo administration of a therapeutic lentiviral vector targeting the expression of a human fumarylacetoacetate hydrolase (FAH) transgene in the porcine model of HT1. This therapy is well tolerated and provides stable long-term expression of FAH in pigs with HT1. Genomic integration displays a benign profile, with subsequent fibrosis and tumorigenicity gene expression patterns similar to wild-type animals as compared to NTBC-treated or diseased untreated animals. Indeed, the phenotypic and genomic data following in vivo lentiviral vector administration demonstrate comparative superiority over other therapies including ex vivo cell therapy and therefore support clinical application of this approach.
Keyphrases
- gene therapy
- cell therapy
- liver fibrosis
- liver failure
- gene expression
- poor prognosis
- wild type
- endothelial cells
- hepatitis b virus
- stem cells
- copy number
- dna methylation
- binding protein
- electronic health record
- big data
- induced pluripotent stem cells
- newly diagnosed
- genome wide
- smoking cessation
- pluripotent stem cells
- artificial intelligence