2001 Fiscal Year Final Research Report Summary
Regulation of T-cell and antigen-presenting cell interactions by Rapl.
Project/Area Number |
12670300
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Research Category |
Grant-in-Aid for Scientific Research (C)
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Allocation Type | Single-year Grants |
Section | 一般 |
Research Field |
Immunology
|
Research Institution | KYOTO UNIVERSITY |
Principal Investigator |
HATTORI Masakazu Kyoto University, Graduate school of Biostudies, Dept. of Immunology and Cell Biology, Associate Professor, 生命科学研究科, 助教授 (40211479)
|
Co-Investigator(Kenkyū-buntansha) |
MINATO Nagahiro Kyoto University, Graduate school of Biostudies, Dept. of Immunology and Cell Biology, Professor, 生命科学研究科, 教授 (40137716)
|
Project Period (FY) |
2000 – 2001
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Keywords | Rap1 / SPA- 1 / T cell / anergy / apoptosis / p27kip1 |
Research Abstract |
Activation of T cells by antigen requires adhesive interactions with antigen-presenting cells (APC) in which leukocyte function-associated antigen 1 (LFA-1) and intercellular adhesion molecules (ICAMs) are important. However, it is not well understood what signaling molecules regulate this process and how the modulation of adhesive events influences T-cell activation. Here we show that Rap1 is activated in T cells in an antigen-dependent manner and accumulated at the contact site of T-cell and antigen-loaded APC. Inhibition of Rap1 activation by a dominant-negative Rap1 or SPA-1, a Rapl GTPase-activating protein, abrogates LFA-1-ICAM-1-mediated adhesive interactions with antigen-pulsed APC and the subsequent T-cell-receptor triggering and interleukin-2 production. Conversely, augmented antigen-dependent Rap1 activation by the expression of wild-type Rap1 enhances these responses but culminates in apoptosis by Fas and FasL. Thus, Rap1 functions as a key regulator of T-cell and APC interactions and modulates T-cell responses from productive activation to activation-induced cell death by regulating the strength of adhesive interactions. Moreover, constitutive Rap1 activation rendered T cells unresponsive with accumulation of p27(Kip1). Our study indicates that the activation state of Rap1 has a decisive effect on the T-cell response to antigen.
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Research Products
(8 results)