24. Sustained Expression with Partial Correction of Neutrophil Defects 5 Years After Intramuscular rAAV1 Gene Therapy for Alpha-1 Antitrypsin Deficiency

Abstract

Alpha-1 antitrypsin (AAT) deficiency is a common monogenic disorder resulting in emphysema, which is currently treated with weekly infusions of protein replacement. We previously reported achieving plasma wild-type (M) AAT concentrations at 2.5-3.8% of the therapeutic level at 1 year after intramuscular (IM) administration of 6×1012vg/kg of a recombinant adeno-associated virus serotype 1 (rAAV1)-AAT vector in AAT-deficient patients, with an associated regulatory T cell (Treg) response to AAV1 capsid epitopes in the absence of any exogenous immune suppression. Here, we report sustained expression, at >2% of the therapeutic level, for 5 years after one-time treatment with rAAV1-AAT in an AAT-deficient patient from that study, with the partial correction of neutrophil defects previously reported in AAT-deficient patients. There was also evidence of an in-situ Treg response and an exhausted CD8+ T cell response to AAV1 capsid. These findings suggest that muscle-based AAT gene replacement is tolerogenic and that very stable levels of M AAT may exert beneficial effects at lower concentrations than previously anticipated.