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2007 Volume No 13
pages 93-99
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Title: Adeno-associated viral vector transduction of
human mesenchymal stem cells
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Author: S Stender, M Murphy, T O'Brien, C Stengaard,
M Ulrich-Vinther, K Søballe, F Barry
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Address: Regenerative Medicine Institute, National
University of Ireland, Galway, Ireland
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E-mail: frank.barry@nuigalway.ie
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Key Words: Mesenchymal stem cells, adeno-associated virus,
transgene expression, multipotential activity
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Publication date: May 31st 2007
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Abstract: Mesenchymal stem cells (MSCs) have received
considerable attention in the emerging field of regenerative
medicine. One aspect of MSC research focuses on genetically
modifying the cells with the aim of enhancing their regenerative
potential. Adeno-associated virus (AAV) holds promise as a
vector for human gene therapy, primarily due to its lack of
pathogenicity and low risk of insertional mutagenesis. However,
the existing data pertaining to AAV transduction of MSCs is
limited.
The objective of this work was to examine the efficiency and
kinetics of in vitro transduction using AAV serotype 2 in
human MSCs and to assess whether AAV transduction affects
MSC multipotentiality. The results indicated that human MSCs
could indeed be transiently transduced in vitro by the AAV2
vector with efficiencies of up to 65%. The percentage of GFP-positive
cells peaked at 4 days post-transduction and declined rapidly
towards 0% after day 8. The level of transgene expression
in the GFP-positive population increased 4-fold over a 10,000
fold viral dose increase. This dose-response contrasted with
the 200-fold increase observed in similarly transduced 293-cells,
indicating a relatively restricted transgene expression in
MSCs following AAV mediated gene delivery. Importantly, transduced
MSCs retained multipotential activity comparable to untransduced
controls.
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