肥満細胞特異的Stat6アイソフォームの発現制御機構とその機能解析

Research Project

Project/Area Number	13770231
Research Category	Grant-in-Aid for Young Scientists (B)
Allocation Type	Single-year Grants
Research Field	内科学一般
Research Institution	Chiba University
Principal Investigator	中島裕史千葉大学, 医学部附属病院, 助手 (00322024)
Co-Investigator(Kenkyū-buntansha)	岩本逸夫千葉大学, 大学院・医学研究院, 助教授 (10111436)
Project Period (FY)	2001 – 2002
Project Status	Completed (Fiscal Year 2002)
Budget Amount *help	¥2,900,000 (Direct Cost: ¥2,900,000) Fiscal Year 2002: ¥1,000,000 (Direct Cost: ¥1,000,000) Fiscal Year 2001: ¥1,900,000 (Direct Cost: ¥1,900,000)
Keywords	肥満細胞 / Stat6切断酵素 / 65kDa Stat6 / 蛋白分解酵素 / セリンプロテアーゼ / Stat5切断酵素 / 核局在 / Stat6 / 蛋白分解 / 細胞死抑制 / レトロウイルス
Research Abstract	本研究者は、種々の血球系細胞におけるcommon cytokine receptorγ鎖(γc)依存性シグナルを解析する過程で、肥満細胞には通常の細胞に発現していない65-kDaのStat6 (65-kDa Stat6)が特異的に発現している事を見出した(Blood 96:2172-2180,2000)。そして、本申請研究では、65kDa Stat6の産生機構及びその生理的意義の解明を目指して研究を行い、1.65-kDa Stat6は、肥満細胞に特異的に存在する切断分解酵素によりStat6のC端が切断されることにより産生されること、2.Stat6切断酵素活性は、肥満細胞の核内に限局していること、3.Stat6切断酵素は、未分化な骨髄球系細胞に存在するStat5切断酵素とは異なること、4.Stat6切断酵素は、セリンプロテアーゼインヒビターにより特異的に阻害されること、5.65-kDa Stat6はIL-4による通常型Stat6の活性化に対して優性抑制性に機能すること、6.Stat6切断酵素に抵抗性を示す変異Stat6をStat6欠損肥満細胞内に発現させると野生型Stat6に比して強い転写活性を有することを見出した(J. Exp. Med. 196,27-38,2002)。すなわち、肥満細胞においては、活性化されたStat6が核内に移行した後にStat6切断酵素により切断をうけ、その結果産生された65-kDa Stat6がIL-4反応性を抑制性に制御するという特異な制御機構が存在することが示唆された。現在、レトロウイルス発現法を用いて肥満細胞ライブラリーから内因性Stat6抑制物質をスクリーニング中である。本スクリーニングによりStat6切断酵素の単離が可能と考える。

Report

(2 results)

2002 Annual Research Report
2001 Annual Research Report

Research Products

(10 results)

All Other

All Publications (10 results)

[Publications] Ikeda K, Nakajima H, Suzuki K, Suto A, Saito Y, Iwamoto I.: "Mast cells produce Interleukin-25 upon FcεRI-mediated acivation"Blood. 100(in press). (2003)
- Related Report
  2002 Annual Research Report
[Publications] Nakajima H, Suzuki K, Kagami S-i, Suto A, Saito Y, Akira S, Iwamoto I.: "Proteolytic processing of Stat6 signaling in mast cells as a negative-regulatory mechanism"J. Exp. Med.. 196. 27-38 (2002)
- Related Report
  2002 Annual Research Report
[Publications] Suto A, Nakajima H, Nakayama T, Taniguchi M, Saito Y, Iwamoto I.: "CD4+CD25+T cell development is regulated by at least two distinct mechanisms"Blood. 99. 555-560 (2002)
- Related Report
  2002 Annual Research Report
[Publications] Kunstle G, Pierron G, Kagami S-i, Nakajima H, Noguchi M.: "Identification of Akt association and oligomerization domeins of the Akt kinase coactivator TCLl"Mol. Cell. Biol.. 22. 1513-1525 (2002)
- Related Report
  2002 Annual Research Report
[Publications] Suto A, et al.: "CD4+CD25+T cell development is regulated by at least two distinct mechanisms"Blood. 99. 555-560 (2002)
- Related Report
  2001 Annual Research Report
[Publications] Kagami S-I, et al.: "Stat5a regulates T helper cell differentiation by several distinct mechanisms"Blood. 97. 2358-2365 (2001)
- Related Report
  2001 Annual Research Report
[Publications] Suto A, et al.: "Role of CD4+CD25+regulatory T cells in T helper 2 cell-mediated allergic inflammation in the airways"Am. J. Respir. Crit. Care Med. 164. 680-687 (2001)
- Related Report
  2001 Annual Research Report
[Publications] Uchida Y, et al.: "Increase of dendritic cell type 2 by altered response to interleukin-4 in atopic patients"J. Allergy Clin. Immunol. 108. 1005-1011 (2001)
- Related Report
  2001 Annual Research Report
[Publications] Goto D, et al.: "Interaction between Smad anchor for receptor activation and Smad3 is not essential for TGF-beta/Smad3-mediated signaling"Biochem Biophys Res Commun. 281. 1100-1105 (2001)
- Related Report
  2001 Annual Research Report
[Publications] Kasai M, et al.: "T cell vaccination eliminates antigen-specific T cells and prevents antigen-induced eosinophil recruitment into the tissue"Int Arch Allergy Immunol. 125. 59-66 (2001)
- Related Report
  2001 Annual Research Report

肥満細胞特異的Stat6アイソフォームの発現制御機構とその機能解析

Principal Investigator

中島 裕史 千葉大学, 医学部附属病院, 助手 (00322024)

¥2,900,000 (Direct Cost: ¥2,900,000)

Report

Research Products

[Publications] Ikeda K, Nakajima H, Suzuki K, Suto A, Saito Y, Iwamoto I.: "Mast cells produce Interleukin-25 upon FcεRI-mediated acivation"Blood. 100(in press). (2003)

Related Report

[Publications] Nakajima H, Suzuki K, Kagami S-i, Suto A, Saito Y, Akira S, Iwamoto I.: "Proteolytic processing of Stat6 signaling in mast cells as a negative-regulatory mechanism"J. Exp. Med.. 196. 27-38 (2002)

Related Report

[Publications] Suto A, Nakajima H, Nakayama T, Taniguchi M, Saito Y, Iwamoto I.: "CD4+CD25+T cell development is regulated by at least two distinct mechanisms"Blood. 99. 555-560 (2002)

Related Report

[Publications] Kunstle G, Pierron G, Kagami S-i, Nakajima H, Noguchi M.: "Identification of Akt association and oligomerization domeins of the Akt kinase coactivator TCLl"Mol. Cell. Biol.. 22. 1513-1525 (2002)

Related Report

[Publications] Suto A, et al.: "CD4+CD25+T cell development is regulated by at least two distinct mechanisms"Blood. 99. 555-560 (2002)

Related Report

[Publications] Kagami S-I, et al.: "Stat5a regulates T helper cell differentiation by several distinct mechanisms"Blood. 97. 2358-2365 (2001)

Related Report

[Publications] Suto A, et al.: "Role of CD4+CD25+regulatory T cells in T helper 2 cell-mediated allergic inflammation in the airways"Am. J. Respir. Crit. Care Med. 164. 680-687 (2001)

Related Report

[Publications] Uchida Y, et al.: "Increase of dendritic cell type 2 by altered response to interleukin-4 in atopic patients"J. Allergy Clin. Immunol. 108. 1005-1011 (2001)

Related Report

[Publications] Goto D, et al.: "Interaction between Smad anchor for receptor activation and Smad3 is not essential for TGF-beta/Smad3-mediated signaling"Biochem Biophys Res Commun. 281. 1100-1105 (2001)

Related Report

[Publications] Kasai M, et al.: "T cell vaccination eliminates antigen-specific T cells and prevents antigen-induced eosinophil recruitment into the tissue"Int Arch Allergy Immunol. 125. 59-66 (2001)

Related Report

中島裕史千葉大学, 医学部附属病院, 助手 (00322024)