Transcription factor decoy for AP-1 reduces
mesangial cell proliferation and extracellular matrix
production in vitro and in vivo
- Author(s)
- JD Ahn; R Morishita; Y Kaneda; HJ Kim; YD Kim; HJ Lee; KU Lee; JY Park; YH Kim; KK Park; YC Chang; KH Yoon; HS Kwon; KG Park; IK Lee
- Keimyung Author(s)
- Park, Keun Gyu; Lee, In Kyu; Park, Kwan Kyu
- Department
- Dept. of Internal Medicine (내과학)
Dept. of Pathology (병리학)
Kidney Institute (신장연구소)
- Journal Title
- Cancer Gene Therapy
- Issued Date
- 2004
- Volume
- 11
- Issue
- 11
- Abstract
- Diabetic nephropathy is characterized by an expansion of
glomerular mesangium, caused by mesangial cell
proliferation and excessive accumulation of extracellular
matrix (ECM) proteins, which eventually leads to glomerulosclerosis
and renal failure. Activator protein-1 (AP-1), a
transcription factor, is implicated in the transcriptional
regulation of a wide range of genes participating in cell
proliferation and ECM production. This investigation was
undertaken to test the hypothesis that AP-1 plays an
important role in ECM gene expression, and to develop a
molecular therapeutic strategy based on decoy oligodeoxynucleotides
(ODN). In this report, we show that transfection
with AP-1 decoy ODN strongly inhibits high glucose- and
angiotensin II-induced cell proliferation and expression of
ECM genes in cultured mesangial cells in vitro. Administration
of AP-1 decoy ODN into streptozotocin-induced diabetic
rat kidney in vivo using the hemagglutinating virus of Japan
(HVJ)-liposome method virtually abolished TGF-b1 and
plasminogen activator inhibitor-1 expression. Our results
collectively indicate that AP-1 activation is crucial for
mesangial cell proliferation and ECM production in response
to high glucose and angiotensin II. Moreover, use of stable
AP-1 decoy ODN combined with the highly effective HVJliposome
method provides a novel potential molecular
therapeutic strategy for the prevention of diabetic nephropathy.
Gene Therapy (2004) 11, 916–923. doi:10.1038/sj.gt.3302236
Published online 12 February 2004
Keywords: mesangial cell; AP-1 decoy ODN; extracellular matrix; high glucose; angiotensin II; proliferation
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