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REGULATION OF PROMER OF TGF-β/SMAD-TARGET GENE FOR ATTENUATION OF RENAL FIBROSIS

Research Project

Project/Area Number 13671132
Research Category

Grant-in-Aid for Scientific Research (C)

Allocation TypeSingle-year Grants
Section一般
Research Field Kidney internal medicine
Research InstitutionKURUME UNIVERSITY

Principal Investigator

TAMAKI Kiyoshi  KURUME UNIVERSITY SCHOOL OF MEDICINE, DEPARTMENT OF NEPHROLOGY, ASSISTANT PROFESSOR, 医学部, 講師 (10312141)

Project Period (FY) 2001 – 2002
Project Status Completed (Fiscal Year 2002)
Budget Amount *help
¥3,600,000 (Direct Cost: ¥3,600,000)
Fiscal Year 2002: ¥1,800,000 (Direct Cost: ¥1,800,000)
Fiscal Year 2001: ¥1,800,000 (Direct Cost: ¥1,800,000)
KeywordsGrowth factor / TGF-β / Smad / renal fibrosis / Smad binding element / Lux / GFP
Research Abstract

TGF-β/Smad-target gene such as plasminogen activator inhibitor has Smad-binding element (SEE) in its promoter region. We generated artificial plasmid consisted of luciferase gene with SBE (SBE-Lux) in its promoter region. Using this plasmid, we have done experiments as follows. Cultured mesangial cells or smooth muscles cells was transfected with the plasmid and the cultured cells were treated with TGF-β or the substances, which are shown to induce the production of TGF-β. TGF-β increased the activity of SBE-Lux in dose-dependent manner. Angiotension II and Advanced glycation end product (AGE) also stimulated SBE-Lux activity. The activity was blocked by the presence of neutralizing anti-TGF-β antibody.
Next, we generated artificial plasmid consisted of GFP (green fluorescence product) gene with SBE (SBE-GFP) in its promoter region. The cells transfected with the construct showed TGF-β-induced green color in its cytoplasma. Thus, the cell showing green fluolorescence was considered as TGF-β-target-cells. However, the cultured cells, which were transfected with the construct and treated with Angiotension II or AGE, have not shown green color enough to be identified. In addition, the tissues, which were transfectected with SBE-GFP, have not shown the green color induced by sclerotic damage. High concentration of TGF-β more than 10^<-2>ng/ml is necessary to induce the green fluolorescence in the transfected cells. Such high concentration of TGF-β was not considered to exist in the physiological or pathological condition. Thus, more sensitive artificial promoter is necessary to detect TGF-β activity.

Report

(3 results)
  • 2002 Annual Research Report   Final Research Report Summary
  • 2001 Annual Research Report
  • Research Products

    (24 results)

All Other

All Publications (24 results)

  • [Publications] Haramaki R, Tamaki K, et al.: "Steroid therapy and urinary transforming growth factor-beta1 in IgA nephropathy"Am J Kidney Dis.. 38(6). 1191-1198 (2001)

    • Description
      「研究成果報告書概要(和文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Kato S, Tamaki K, et al.: "Ectopic expression of Smad7 inhibits transforming growth factor-beta responses in vascular smooth muscle cells"Life Sci.. 69(229). 2641-2652 (2001)

    • Description
      「研究成果報告書概要(和文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Tamaki K, et al.: "Chinese herbs nephropathy : a variant form in Japan"Intern Med.. 40(4). 267-268 (2001)

    • Description
      「研究成果報告書概要(和文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Fukami K, Tamaki K, et al.: "Advanced Glycation Endproducts and their receptor interactoion promotes mesangial cell damage via angiotensin II and TGF-β"J Am Soc Nephrol. 13. 654A (2002)

    • Description
      「研究成果報告書概要(和文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] K.Tamaki et al.: "Role of TGF-β in the progression of renal fibrosis"Contribution to Nephrology. 139. 44-65 (2003)

    • Description
      「研究成果報告書概要(和文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Ikedo H, Tamaki K et al.: "Smad protein and TGF-β signaling in vascular smooth muscle cells"International Journal of Molecular Medicine. 11. 645-650 (2003)

    • Description
      「研究成果報告書概要(和文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Tamai O, Tamaki K, Okuda S et al: "Caveolae in mesangial cells and caveolin expression in mesangial proliferative glomerulonephritis"Kidney Int.. 59. 471-480 (2001)

    • Description
      「研究成果報告書概要(欧文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Haramaki R, Tamaki K. et al.: "Steroid therapy and urinary transforming growth factor-beta1 in IgA nephropathy"Am J Kidney Dis.. 38. 1191-1198 (2001)

    • Description
      「研究成果報告書概要(欧文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Kato S, Tamaki K, et al.: "Ectopic expression of Smad7 inhibits transforming growth factor-beta responses in vascular smooth"Life Sci.. 69. 2641-2652 (2001)

    • Description
      「研究成果報告書概要(欧文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Fukami K, Tamaki K, et al.: "Advanced Glycation Endproducts receptor and their receptor promotes mesangial cell damage via angiotensin II and TGF-β"J Am Soc Nephrol 2002. 13. 654A (2002)

    • Description
      「研究成果報告書概要(欧文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Ikedo H, Tamaki K, et al.: "Smad protein and TGF-β signaling in vascular smooth muscle cells"International Journal of Molecular Medicine. (in press). (2003)

    • Description
      「研究成果報告書概要(欧文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] Tamaki K, Okuda S: "Role of TGF-β in the progression of renal fibrosis"Contribution to Nephrology. 139. 44-65 (2003)

    • Description
      「研究成果報告書概要(欧文)」より
    • Related Report
      2002 Final Research Report Summary
  • [Publications] K.Tamaki et al.: "Role of TGF-β in the progression of renal fibrosis"Contribution to Nephrology. 139. 44-65 (2003)

    • Related Report
      2002 Annual Research Report
  • [Publications] Ikedo H, Tamaki K et al.: "Smad protein and TGF-β signaling in vascular smooth muscle cells"International Journal of Molecular Medicine. (印刷中). (2003)

    • Related Report
      2002 Annual Research Report
  • [Publications] Fukami K, Tamaki K, et al.: "Advanced Glycation Endproducts and their receptor interactoion promotes mesangial cell damage via angiotensin II and TGF-β"J Am Soc Nephrol. 13. 654A (2002)

    • Related Report
      2002 Annual Research Report
  • [Publications] 玉置清志 他: "急速進行性糸球体腎炎"内科学会雑誌. 91. 1570-1582 (2002)

    • Related Report
      2002 Annual Research Report
  • [Publications] 玉置清志 他: "腎疾患-state of ares 2003-2005"メサンギウム増殖性腎炎のモデル. 232-235 (2003)

    • Related Report
      2002 Annual Research Report
  • [Publications] Haramaki R, Tamaki K, et al.: "Steroid therapy and urinary transforming growth factor-betal in IgA nephropathy"Am J Kidney Dis.. 38(6). 1191-1198 (2001)

    • Related Report
      2001 Annual Research Report
  • [Publications] Kato S, Tamaki K, et al.: "Ectopic expression of Smad7 inhibits transforming growth factor-beta responses in vascular smooth muscle cells"Life Sci.. 69(229). 2641-2652 (2001)

    • Related Report
      2001 Annual Research Report
  • [Publications] Ueda S, Tamaki K, et al.: "Overexpression of Smad7 not Smad6 inhibits TGF-β actions in mesangial cells"A J Soc Nephrol. 623A. (2001)

    • Related Report
      2001 Annual Research Report
  • [Publications] Tamaki K, et al.: "Chinese herbs nephropathy : a variant form in Japan"Intern Med.. 40(4). 267-268 (2001)

    • Related Report
      2001 Annual Research Report
  • [Publications] Tamaki K, Okuda S: "Role of TGB-β in the progression of renal fibrosis"Indian review of renal fibrosis. (印刷中). (2001)

    • Related Report
      2001 Annual Research Report
  • [Publications] 玉置清志 他: "糸球体病変と成長因子、ケモカイン"内科. 87(6). (2001)

    • Related Report
      2001 Annual Research Report
  • [Publications] 奥田誠也 他: "腎と透析、51、臨時増刊"糖尿病性腎症におけるTGF-βの役割. 162-167 (2001)

    • Related Report
      2001 Annual Research Report

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Published: 2001-04-01   Modified: 2016-04-21  

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