Vector Design Influences Hepatic Genotoxicity After Adeno-associated Virus Gene Therapy

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2015 Jan 22

PMID 25607839

Citations 202

Authors

Randy J Chandler

Matthew C LaFave

Gaurav K Varshney

Niraj S Trivedi

Nuria Carrillo-Carrasco

Julien S Senac

Weiwei Wu

Victoria Hoffmann

Abdel G Elkahloun

Shawn M Burgess

Charles P Venditti

Affiliations

Soon will be listed here.

Abstract

The use of adeno-associated virus (AAV) as a gene therapy vector has been approved recently for clinical use and has demonstrated efficacy in a growing number of clinical trials. However, the safety of AAV as a vector has been challenged by a single study that documented hepatocellular carcinoma (HCC) after AAV gene delivery in mice. Most studies have not noted genotoxicity following AAV-mediated gene delivery; therefore, the possibility that there is an association between AAV and HCC is controversial. Here, we performed a comprehensive study of HCC in a large number of mice following therapeutic AAV gene delivery. Using a sensitive high-throughput integration site-capture technique and global expressional analysis, we found that AAV integration into the RNA imprinted and accumulated in nucleus (Rian) locus, and the resulting overexpression of proximal microRNAs and retrotransposon-like 1 (Rtl1) were associated with HCC. In addition, we demonstrated that the AAV vector dose, enhancer/promoter selection, and the timing of gene delivery are all critical factors for determining HCC incidence after AAV gene delivery. Together, our results define aspects of AAV-mediated gene therapy that influence genotoxicity and suggest that these features should be considered for design of both safer AAV vectors and gene therapy studies.

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