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scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints

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 AAV-mediated gene transfer to large, weight-bearing human joints. A self-complementary AAV2 vector containing the coding regions for human interleuki...

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Autores principales: Watson, Rachael S., Broome, Ted A., Levings, Padraic P., Rice, Bret L., Kay, Jesse D., Smith, Andrew D., Gouze, Elvire, Gouze, Jean-Noel, Dacanay, E. Anthony, Hauswirth, William W., Nickerson, David M., Dark, Michael J., Colahan, Patrick T., Ghivizzani, Steven C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3577988/
https://www.ncbi.nlm.nih.gov/pubmed/23151520
http://dx.doi.org/10.1038/gt.2012.81
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author Watson, Rachael S.
Broome, Ted A.
Levings, Padraic P.
Rice, Bret L.
Kay, Jesse D.
Smith, Andrew D.
Gouze, Elvire
Gouze, Jean-Noel
Dacanay, E. Anthony
Hauswirth, William W.
Nickerson, David M.
Dark, Michael J.
Colahan, Patrick T.
Ghivizzani, Steven C.
author_facet Watson, Rachael S.
Broome, Ted A.
Levings, Padraic P.
Rice, Bret L.
Kay, Jesse D.
Smith, Andrew D.
Gouze, Elvire
Gouze, Jean-Noel
Dacanay, E. Anthony
Hauswirth, William W.
Nickerson, David M.
Dark, Michael J.
Colahan, Patrick T.
Ghivizzani, Steven C.
author_sort Watson, Rachael S.
collection PubMed
description 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 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 (GFP) 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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spelling pubmed-35779882013-12-01 scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints Watson, Rachael S. Broome, Ted A. Levings, Padraic P. Rice, Bret L. Kay, Jesse D. Smith, Andrew D. Gouze, Elvire Gouze, Jean-Noel Dacanay, E. Anthony Hauswirth, William W. Nickerson, David M. Dark, Michael J. Colahan, Patrick T. Ghivizzani, Steven C. Gene Ther Article 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 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 (GFP) 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. 2012-11-15 2013-06 /pmc/articles/PMC3577988/ /pubmed/23151520 http://dx.doi.org/10.1038/gt.2012.81 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Watson, Rachael S.
Broome, Ted A.
Levings, Padraic P.
Rice, Bret L.
Kay, Jesse D.
Smith, Andrew D.
Gouze, Elvire
Gouze, Jean-Noel
Dacanay, E. Anthony
Hauswirth, William W.
Nickerson, David M.
Dark, Michael J.
Colahan, Patrick T.
Ghivizzani, Steven C.
scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints
title scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints
title_full scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints
title_fullStr scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints
title_full_unstemmed scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints
title_short scAAV-Mediated Gene Transfer of Interleukin 1-Receptor Antagonist to Synovium and Articular Cartilage in Large Mammalian Joints
title_sort scaav-mediated gene transfer of interleukin 1-receptor antagonist to synovium and articular cartilage in large mammalian joints
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3577988/
https://www.ncbi.nlm.nih.gov/pubmed/23151520
http://dx.doi.org/10.1038/gt.2012.81
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