Dillon Tara J, Carey Kendall D, Wetzel Scott A, Parker David C, Stork Philip J S
Vollum Institute, Oregon Health & Science University, Portland, Oregon 97239, USA.
Mol Cell Biol. 2005 May;25(10):4117-28. doi: 10.1128/MCB.25.10.4117-4128.2005.
The mitogen-activated protein kinase extracellular signal-regulated kinase (ERK) is activated following engagement of the T-cell receptor and is required for interleukin 2 (IL-2) production and T-cell proliferation. This activation is enhanced by stimulation of the coreceptor CD28 and inhibited by the coreceptor CTLA-4. We show that the small G protein Rap1 is regulated in the opposite manner; it is inhibited by CD28 and activated by CTLA-4. Together, CD3 and CTLA-4 activate Rap1 in a sustained manner. To delineate T-cell function in the absence of Rap1 activity, we generated transgenic mice expressing Rap1GAP1, a Rap1-specific GTPase-activating protein. Transgenic mice showed lymphadenopathy, and transgenic T cells displayed increased ERK activation, proliferation, and IL-2 production. More significantly, the inhibitory effect of CTLA-4 on T-cell function in Rap1GAP1-transgenic T cells was reduced. We demonstrate that CTLA-4 activates Rap1, and we propose that intracellular signals from CTLA-4 antagonize CD28, at least in part, at the level of Rap1.
丝裂原活化蛋白激酶细胞外信号调节激酶(ERK)在T细胞受体结合后被激活,是白细胞介素2(IL-2)产生和T细胞增殖所必需的。共刺激分子CD28的刺激可增强这种激活,而共刺激分子CTLA-4则抑制这种激活。我们发现小G蛋白Rap1的调节方式相反;它被CD28抑制,被CTLA-4激活。CD3和CTLA-4共同持续激活Rap1。为了阐明在没有Rap1活性的情况下T细胞的功能,我们构建了表达Rap1特异性GTP酶激活蛋白Rap1GAP1的转基因小鼠。转基因小鼠出现淋巴结病,转基因T细胞表现出增强的ERK激活、增殖和IL-2产生。更显著的是,CTLA-4对Rap1GAP1转基因T细胞中T细胞功能的抑制作用减弱。我们证明CTLA-4激活Rap1,并提出来自CTLA-4的细胞内信号至少部分地在Rap1水平上拮抗CD28。
