Hepatic expression of GAA results in enhanced enzyme bioavailability in mice and non-human primates.
Helena Costa-VerderaFanny CollaudChristopher R RilingPauline SellierJayme M L NordinG Michael PrestonUmut CaginJulien FabregueSimon BarralMaryse Moya-NilgesJacomina Krijnse-LockerLaetitia van WittenbergheNatalie DanieleBernard GjataJeremie CosetteCatalina AbadMarcelo Simon-SolaSeverine CharlesMathew LiMarco CrosariolTom AntrilliWilliam J QuinnDavid A GrossOlivier BoyerXavier M AnguelaSean M ArmourPasqualina ColellaGiuseppe RonzittiFederico MingozziPublished in: Nature communications (2021)
Pompe disease (PD) is a severe neuromuscular disorder caused by deficiency of the lysosomal enzyme acid alpha-glucosidase (GAA). PD is currently treated with enzyme replacement therapy (ERT) with intravenous infusions of recombinant human GAA (rhGAA). Although the introduction of ERT represents a breakthrough in the management of PD, the approach suffers from several shortcomings. Here, we developed a mouse model of PD to compare the efficacy of hepatic gene transfer with adeno-associated virus (AAV) vectors expressing secretable GAA with long-term ERT. Liver expression of GAA results in enhanced pharmacokinetics and uptake of the enzyme in peripheral tissues compared to ERT. Combination of gene transfer with pharmacological chaperones boosts GAA bioavailability, resulting in improved rescue of the PD phenotype. Scale-up of hepatic gene transfer to non-human primates also successfully results in enzyme secretion in blood and uptake in key target tissues, supporting the ongoing clinical translation of the approach.
Keyphrases
- replacement therapy
- endothelial cells
- poor prognosis
- mouse model
- genome wide
- copy number
- gene expression
- recombinant human
- smoking cessation
- gene therapy
- induced pluripotent stem cells
- pluripotent stem cells
- type diabetes
- dna methylation
- oxidative stress
- molecular docking
- skeletal muscle
- heat shock
- high fat diet induced
- heat shock protein
- wild type