Effects of glucose and plasminogen activator inhibitor-1 on collagen metabolism in the peritoneum
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Higuchi, C
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Tokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, JapanTokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, Japan
Higuchi, C
[1
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Tanihata, Y
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Tokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, JapanTokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, Japan
Tanihata, Y
[1
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Nishimura, H
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Tokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, JapanTokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, Japan
Nishimura, H
[1
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Naito, T
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Tokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, JapanTokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, Japan
Naito, T
[1
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Sanaka, T
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Tokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, JapanTokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, Japan
Sanaka, T
[1
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[1] Tokyo Womens Med Univ, Daini Hosp, Div Internal Med, Arakawa Ku, Tokyo, Japan
Nonphysiological solutions containing high glucose levels have been considered an important factor in the etiology of fibrotic changes in long-term continuous ambulatory peritoneal dialysis (CAPD) patients. At the same time, increased Plasminogen Activator Inhibitor (PAI)-1 secretion has been reported to correlate with fibrotic changes. We suspected that the high glucose content of peritoneal dialysis solution may induce peritoneal sclerosis via up-regulation of PAI-1 gene expression. In this study, we evaluated the effects of glucose on PAI-1 activity in peritoneal fibrosis in a rat model of CAPD. The effects of glucose on the expressions of PAI-1 and several other genes correlated with collagen metabolism were also examined in cultured rat peritoneal mesothelial cells and fibroblasts. Sprague-Dawley rats were intraperitone ally injected twice daily for 28 days with phosphate-buffered saline (PBS) (control group), PBS containing 4% glucose (glucose group), or PBS containing 4% glucose plus a PAI-1. inhibitor (PAI-1 inhibitor group). Thickening of the peritoneum with increase the deposition of collagens type I and III in the submesothelial interstitium were observed in the glucose and the PAI-1 inhibitor group, but these were less severe in the PAI-1 inhibitor group. Glucose stimulated expression of the mRNA of PAI-1, collagen type I and III, and tissue inhibitor of metalloproteinase (TIMP)-1 in fibroblasts but not in mesothelial cells. Glucose stimulated matrix metalloproteinase (MMP)-13 mRNA expression in both cell types. The PAI-1 inhibitor suppressed expression of the mRNAs induced by glucose. In conclusion, glucose induces peritoneal fibrosis, including changes in collagen metabolism, by stimulating PAI-1 expression.
机构:
Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Univ Ottawa, Inst Heart, Vasc Biol & Expt Med Lab, Ottawa, ON, Canada
Univ Ottawa, Dept Cellular & Mol Med, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Jung, Richard G.
Simard, Trevor
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Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Univ Ottawa, Inst Heart, Vasc Biol & Expt Med Lab, Ottawa, ON, Canada
Univ Ottawa, Dept Cellular & Mol Med, Ottawa, ON, Canada
Univ Ottawa, Inst Heart, Div Cardiol, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Simard, Trevor
Labinaz, Alisha
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Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Labinaz, Alisha
Ramirez, F. Daniel
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Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Univ Ottawa, Inst Heart, Div Cardiol, Ottawa, ON, Canada
Univ Ottawa, Sch Epidemiol Publ Hlth & Prevent Med, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Ramirez, F. Daniel
Di Santo, Pietro
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Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Univ Ottawa, Inst Heart, Div Cardiol, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Di Santo, Pietro
Motazedian, Pouya
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Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Motazedian, Pouya
Rochman, Rebecca
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Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Univ Ottawa, Inst Heart, Vasc Biol & Expt Med Lab, Ottawa, ON, Canada
Univ Ottawa, Inst Heart, Div Cardiol, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Rochman, Rebecca
Gaudet, Chantal
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Univ Ottawa, Inst Heart, Vasc Biol & Expt Med Lab, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Gaudet, Chantal
Faraz, Mohammad Ali
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Univ Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada
Faraz, Mohammad Ali
Beanlands, Rob S. B.
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Univ Ottawa, Inst Heart, Div Cardiol, Ottawa, ON, CanadaUniv Ottawa, Inst Heart, CAPITAL Res Grp, Ottawa, ON, Canada