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Role of chimaerins, a group of Rac-specific GTPase activating proteins, in T-cell receptor signaling

机译:Chimaerins是一组Rac特异性GTPase激活蛋白,在T细胞受体信号传导中的作用

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摘要

Chimaerins are GTPase-activating proteins that inactivate the GTP-hydrolase Rac1 in a diacylglycerol-dependent manner. To date, the study of chimaerins has been done mostly in neuronal cells. Here, we show that α2- and β2-chimaerin are expressed at different levels in T-cells and that they participate in T-cell receptor signaling. In agreement with this, we have observed that α2- and β2-chimaerins translocate to the T-cell/B-cell immune synapse and, using both gain- and loss-of-function approaches, demonstrated that their catalytic activity is important for the inhibition of the T-cell receptor- and Vav1-dependent stimulation of the transcriptional factor NF-AT. Mutagenesis-based approaches have revealed the molecular determinants that contribute to the biological program of chimaerins during T-cell responses. Unexpectedly, we have found that the translocation of chimaerins to the T-cell/B-cell immune synapse does not rely on the canonical binding of diacylglycerol to the C1 region of these GTPase-activating proteins. Taken together, these results identify chimaerins as candidates for the downmodulation of Rac1 in T-lymphocytes and, in addition, uncover a novel regulatory mechanism that mediates their activation in T-cells. © 2007 Elsevier Inc. All rights reserved.
机译:Chimaerins是GTPase激活蛋白,可以以依赖于二酰基甘油的方式使GTP水解酶Rac1失活。迄今为止,对chimaerins的研究主要是在神经元细胞中进行的。在这里,我们显示α2-和β2-chimaerin在T细胞中以不同的水平表达,并且它们参与T细胞受体信号传导。与此相符,我们已经观察到α2-和β2-chimaerins易位至T细胞/ B细胞免疫突触,并使用功能获得和丧失功能方法证明它们的催化活性对抑制转录因子NF-AT的T细胞受体依赖性和Vav1依赖性刺激。基于诱变的方法已经揭示了在T细胞应答过程中有助于chimaerins生物学程序的分子决定簇。出乎意料的是,我们已经发现,chimaerins到T细胞/ B细胞免疫突触的易位并不依赖于二酰基甘油与这些GTPase激活蛋白的C1区的典型结合。综上所述,这些结果确定了chimaerins作为T淋巴细胞中Rac1的下调候选物,此外,还发现了介导其在T细胞中激活的新型调节机制。 ©2007 Elsevier Inc.保留所有权利。

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