ScAAV-mediated Gene Transfer of Interleukin-1-receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints

Overview

Journal Gene Ther

Date 2012 Nov 16

PMID 23151520

Citations 33

Authors

R S Watson

T A Broome

P P Levings

B L Rice

J D Kay

A D Smith

E Gouze

J-N Gouze

E A Dacanay

W W Hauswirth

D M Nickerson

M J Dark

P T Colahan

S C Ghivizzani

Affiliations

Soon will be listed here.

Abstract

With the long-term goal of developing a gene-based treatment for osteoarthritis (OA), we performed studies to evaluate the equine joint as a model for adeno-associated virus (AAV)-mediated gene transfer to large, weight-bearing human joints. A self-complementary AAV2 vector containing the coding regions for human interleukin-1-receptor antagonist (hIL-1Ra) or green fluorescent protein was packaged in AAV capsid serotypes 1, 2, 5, 8 and 9. Following infection of human and equine synovial fibroblasts in culture, we found that both were only receptive to transduction with AAV1, 2 and 5. For these serotypes, however, transgene expression from the equine cells was consistently at least 10-fold higher. Analyses of AAV surface receptor molecules and intracellular trafficking of vector genomes implicate enhanced viral uptake by the equine cells. Following delivery of 1 × 10(11) vector genomes of serotypes 2, 5 and 8 into the forelimb joints of the horse, all three enabled hIL-1Ra expression at biologically relevant levels and effectively transduced the same cell types, primarily synovial fibroblasts and, to a lesser degree, chondrocytes in articular cartilage. These results provide optimism that AAV vectors can be effectively adapted for gene delivery to large human joints affected by OA.

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