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2005 Volume No 10
pages 40-50
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Title: Adeno-Associated Vector mediated gene transfer
of Transforming Growth Factor -beta1 to normal and osteoarthritic
human chondrocytes stimulates cartilage anabolism
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Authors: M Ulrich-Vinther, C Stengaard, EM Schwarz,
MB Goldring, K Soballe
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Address: Department of Orthopaedics, Aarhus University
Hospital, Tage Hansens Gade 2,
DK-8000 Aarhus C, Denmark
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E-mail: ulrich-vinther@mail.dk
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Key Words: Adeno-Associated Virus, Transforming Growth
Factor-beta1, gene therapy, cartilage, osteoarthritis
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Publication date: November 14th 2005
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Abstract: The objective of the present study was
to investigate whether cartilage anabolism in human primary
osteoarthritic chondrocytes could be improved by adeno-associated
virus (AAV) vector-mediated gene transduction of transforming
growth factor TGF-beta1 (TGF-beta1).
A bi-cistronic AAV-TGF-beta1-IRES-eGFP (AAV-TGF-beta1) vector
was generated and used for transduction of a normal human
articular chondrocyte cell line (tsT/AC62) and primary human
osteoarthritic articular chondrocytes harvested from 8 patients
receiving total knee joint arthroplasty. Transduction efficiency
was detected by fluorescent microscopy for gene expression
of enhanced green fluorescent protein (eGFP). TGF-beta1 synthesis
was determined by ELISA. To assess the influence of TGF-beta1
gene therapy on chondrocyte cartilage metabolism, mRNA expressions
of type II collagen, aggrecan, and matrix metalloproteinase
3 (MMP-3) were determined by quantitative real-time PCR.
AAV-TGF-beta1 transduction resulted in increased synthesis
of TGF-beta1 in both osteoarthritic chondrocytes and the normal
articular chondrocyte cell line. The expression levels of
the transduced genes were correlated to "multiplicity
of infection" (MOI) and post-infectious time. In both
osteoarthritic chondrocytes and the normal articular chondrocyte
cell line, AAV-TGF-beta1 treatment increased mRNA expression
of both type II collagen and aggrecan, but decreased MMP-3
mRNA expression. Osteoarthritic chondrocytes and the normal
articular chondrocyte cell line could be transduced with equal
efficiencies.
In conclusion, it was demonstrated that AAV-TGF-beta1 gene
transfer stimulates cartilage anabolism and decreases expression
of enzymes responsible for cartilage degradation in human
osteoarthritic chondrocytes. The results indicate that the
AAV vector is an efficient mediator of growth factors to human
articular chondrocytes, and that it might be useful in future
chondrocyte gene therapy.
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