Safety of intravenous administration of an AAV8 vector coding for an oxidation-resistant human a1-antitrypsin for the treatment of a1-antitrypsin deficiency Journal Article

   

Authors:	Rosenberg, J. B.; De, B. P.; Greco, A.; Gorman, N.; Kooner, V.; Chen, A.; Yost-Bido, M.; Munoz-Zuluaga, C.; Kaminsky, S. M.; Rostami, M.; Monette, S.; Crystal, R. G.; Sondhi, D.
Article Title:	Safety of intravenous administration of an AAV8 vector coding for an oxidation-resistant human a1-antitrypsin for the treatment of a1-antitrypsin deficiency
Abstract:	a1-antitrypsin (AAT) deficiency is a common autosomal recessive hereditary disorder, with a high risk for the development of early-onset panacinar emphysema. AAT, produced primarily in the liver, functions to protect the lung from neutrophil protease; with AAT deficiency, unimpeded neutrophil proteases destroy the lung parenchyma. AAT is susceptible to oxidative damage resulting in an inability to inhibit its target proteases, neutrophil elastase, and cathepsin G. The major sites of oxidative modification on the AAT molecule are methionine residues 351 and 358. We have previously demonstrated that an engineered variant of AAT that resists oxidation by modifying both protein surface methionines (M351V and M358L) provides antiprotease protection, despite oxidative stress. In mice, intravenous delivery of the modified AAT(AVL) variant by AAV serotype 8, AAV8hAAT(AVL), primarily to the liver resulted in long-term expression of an AAT that resists oxidative inactivation. In this study, we evaluated the safety of intravenous administration of AAV8hAAT(AVL) in a dose-escalating, blinded, placebo-controlled toxicology study in wild-type mice. The study assessed organ histology and clinical pathology findings of mice, intravenously administered AAV8hAAT(AVL) at three doses (5.0 · 1011, 5.0 · 1012, and 5.0 · 1013 genome copies [gc]/kg), compared to control mice injected intravenously with phosphate-buffered saline. As previously demonstrated, administration of AAV8hAAT(AVL) resulted in dose-dependent expression of high, potentially therapeutic, levels of serum human AAT protein that persist for at least 6 months. Antibodies against the AAV8 capsid were elicited as expected, but there was no antibody detected against the AAT(AVL) protein generated by the AAV8hAAT(AVL) vector. There was no morbidity or mortality observed in the study. The data demonstrate that intravenous administration of AAV8hAAT(AVL) is safe with no significant adverse effect attributed to AAV8hAAT(AVL) vector at any dose. This study demonstrates that AAV8hAAT(AVL) has a safety profile consistent with the requirements for proceeding to a clinical study. a 2023 by Mary Ann Liebert, Inc.
Keywords:	genetics; mouse; animal; metabolism; animals; mice; lung; antibodies; antibody; intravenous drug administration; alpha 1 antitrypsin; lung emphysema; alpha 1-antitrypsin; pulmonary emphysema; administration, intravenous; alpha 1 antitrypsin deficiency; humans; human; safety study; a1-antitrypsin deficiency; aav gene therapy; ind-enabling study; oxidation-resistant a1-antitrypsin; toxicology study; alpha 1-antitrypsin deficiency
Journal Title:	Human Gene Therapy
Volume:	34
Issue:	3-4
ISSN:	1043-0342
Publisher:	Mary Ann Liebert, Inc
Date Published:	2023-02-01
Start Page:	139
End Page:	149
Language:	English
DOI:	10.1089/hum.2022.192
PUBMED:	36606685
PROVIDER:	scopus
PMCID:	PMC9963503
DOI/URL:	https://www.scopus.com/inward/record.uri?eid=2-s2.0-85148265235&doi=10.1089%2fhum.2022.192&partnerID=40&md5=203d06014ab2acce1323d76d708fe68b
Notes:	Article -- Export Date: 1 March 2023 -- Source: Scopus

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