2008 Fiscal Year Final Research Report

Signaling mechanism of antiproliferative effect of HGF on carcinoma cells

Research Project

Project/Area Number	19570124
Research Category	Grant-in-Aid for Scientific Research (C)
Allocation Type	Single-year Grants
Section	一般
Research Field	Functional biochemistry
Research Institution	Tokyo Institute of Technology
Principal Investigator	TANAKA Toshiaki Tokyo Institute of Technology, 大学院・生理工学研究科, 助教 (40263446)
Project Period (FY)	2007 – 2008
Keywords	肝細胞増殖因子 / 癌 / HepG2 / 癌抑制因子 / p16 / Id1 / 不可逆的増殖停止
Research Abstract	HGF による肝癌細胞株HepG2の増殖抑制の鍵となるErkの強活性化には、HGF受容体c-Metにアダプター因子Grb2とGab1が結合することが必要であることを明らかにした。また、HGF刺激により転写制御因子Id1の発現量が減少し、それにより癌抑制因子p16が発現上昇することを見出した。Id1とp16は不可逆的細胞変化である細胞老化に係わることから、HGF刺激が不可逆的増殖停止を誘導する可能性を検討した結果、48時間以上のHGF刺激によりHepG2細胞の増殖停止が不可逆的になることを見出した。この結果は、HGF刺激により癌細胞が癌細胞でなくなることを示す重大な発見となった。

Research Products
(5 results)

All 2008 2007 Other

All Journal Article (3 results) (of which Peer Reviewed: 3 results) Presentation (2 results)

[Journal Article] Up-regulation of p21^<CIP1> expressionmediated by ERK-dependent and-independent pathways contributes tohepatocyte growth factor inducedinhibition of HepG2 hepatoma cellproliferation2008
- Author(s)
  E.Shirako, N.Hirayama, Y.Tsukada,T.Tanaka and N.Kitamura
- Journal Title
  
  J.Cell.Biochem 104
  
  Pages: 176-188
- Peer Reviewed
[Journal Article] Coupling of Grb2 to Gab1 mediateshepatocyte growth factor-induced highintensity ERK signal required forinhibition of HepG2 hepatoma cellproliferation2008
- Author(s)
  A.Kondo, N.Hirayama, Y.Sugito, M.Shono,T.Tanaka and N.Kitamura
- Journal Title
  
  J.Biol.Chem 283
  
  Pages: 1428-1436
- Peer Reviewed
[Journal Article] Id1 is downregulated byhepatocyte growth factor viaERK-dependent and-independent signalingpathways, leading to increased expressionof p16INK4a in hepatoma cells
- Author(s)
  K.Ushio, T.Hashimoto, N.Kitamura and T.Tanaka
- Journal Title
  
  Mol.CancerRes (in press)
- Peer Reviewed
[Presentation] 肝癌細胞株HepG2における肝細胞増殖因子HGFによるp16^<INK4a> 発現制御の分子機構2007
- Author(s)
  潮和敬、喜多村直実、田中利明
- Organizer
  第30回日本分子生物学会年会・第80回日本生化学会大会合同大会
- Place of Presentation
  於 : パシフィコ横浜、ヨコハマグランドインターコンチネンタルホテル
- Year and Date
  2007-12-11
[Presentation] Mechanism ofHGF-induced upregulation of p16INK4a inHepG2 hepatoma cells2007
- Author(s)
  Kazutaka Ushio, Naomi Kitamura and Toshiaki Tanaka
- Organizer
  The Toin International Symposium on Biomedical Engineering Engineering 2007
- Place of Presentation
  於 : 桐蔭横浜大学
- Year and Date
  2007-11-02

2008 Fiscal Year Final Research Report

Signaling mechanism of antiproliferative effect of HGF on carcinoma cells

Principal Investigator

TANAKA Toshiaki Tokyo Institute of Technology, 大学院・生理工学研究科, 助教 (40263446)

Research Products

[Journal Article] Up-regulation of p21^<CIP1> expressionmediated by ERK-dependent and-independent pathways contributes tohepatocyte growth factor inducedinhibition of HepG2 hepatoma cellproliferation2008

Author(s)

Journal Title

[Journal Article] Coupling of Grb2 to Gab1 mediateshepatocyte growth factor-induced highintensity ERK signal required forinhibition of HepG2 hepatoma cellproliferation2008

Author(s)

Journal Title

[Journal Article] Id1 is downregulated byhepatocyte growth factor viaERK-dependent and-independent signalingpathways, leading to increased expressionof p16INK4a in hepatoma cells

Author(s)

Journal Title

[Presentation] 肝癌細胞株HepG2における肝細胞増殖因子HGFによるp16^<INK4a> 発現制御の分子機構2007

Author(s)

Organizer

Place of Presentation

Year and Date

[Presentation] Mechanism ofHGF-induced upregulation of p16INK4a inHepG2 hepatoma cells2007

Author(s)

Organizer

Place of Presentation

Year and Date