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文書・図像類

癌抑制G蛋白共役型受容体S1P2の作用機構の研究

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癌抑制G蛋白共役型受容体S1P2の作用機構の研究

Material type
文書・図像類
Author
多久和, 典子ほか
Publisher
-
Publication date
2010-02-03
Material Format
Digital
Capacity, size, etc.
-
NDC
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Note (General):

金沢大学医薬保健研究域医学系G蛋白共役型受容体(GPCR)はあらゆる受容体のうち最大のファミリーを構成しており、現在使用されている医薬品の重要な標的分子である。我々がクローニングし、スフィンゴシン-1-リン酸(S1P)を生理的リガンドとすることを同定したGPCR S1P_2受容体は、G_<12/13...

Related materials as well as pre- and post-revision versions

https://kaken.nii.ac.jp/search/?qm=70150290

https://kaken.nii.ac.jp/grant/KAKENHI-PROJECT-18590259/

https://kaken.nii.ac.jp/report/KAKENHI-PROJECT-18590259/185902592007kenkyu_seika_hokoku_gaiyo/

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  • Kanazawa University Repository for Academic Resources

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Digital

Material Type
文書・図像類
Author/Editor
多久和, 典子
Takuwa, Noriko
Publication Date
2010-02-03
Publication Date (W3CDTF)
2010-02-03
Alternative Title
Molecular mechanisums for S1P_2 G protein coupled receptor-mediated inhibition of tumor progression
Periodical title
平成19(2007)年度 科学研究費補助金 基盤研究(C) 研究成果報告書概要 = 2007 Fiscal Year Final Research Report Summary
No. or year of volume/issue
2006-2007
Volume
2006-2007