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T细胞受体低级别刺激后,Jurkat T细胞中的Ras激活对N-Ras具有特异性,且仅发生在高尔基体上。

Ras activation in Jurkat T cells following low-grade stimulation of the T-cell receptor is specific to N-Ras and occurs only on the Golgi apparatus.

作者信息

Perez de Castro Ignacio, Bivona Trever G, Philips Mark R, Pellicer Angel

机构信息

Department of Pathology and New York University Cancer Institute, New York, New York 10016, USA.

出版信息

Mol Cell Biol. 2004 Apr;24(8):3485-96. doi: 10.1128/MCB.24.8.3485-3496.2004.

Abstract

Ras activation is critical for T-cell development and function, but the specific roles of the different Ras isoforms in T-lymphocyte function are poorly understood. We recently reported T-cell receptor (TCR) activation of ectopically expressed H-Ras on the the Golgi apparatus of T cells. Here we studied the isoform and subcellular compartment specificity of Ras signaling in Jurkat T cells. H-Ras was expressed at much lower levels than the other Ras isoforms in Jurkat and several other T-cell lines. Glutathione S-transferase-Ras-binding domain (RBD) pulldown assays revealed that, although high-grade TCR stimulation and phorbol ester activated both N-Ras and K-Ras, low-grade stimulation of the TCR resulted in specific activation of N-Ras. Surprisingly, whereas ectopically expressed H-Ras cocapped with the TCRs in lipid microdomains of the Jurkat plasma membrane, N-Ras did not. Live-cell imaging of Jurkat cells expressing green fluorescent protein-RBD, a fluorescent reporter of GTP-bound Ras, revealed that N-Ras activation occurs exclusively on the Golgi apparatus in a phospholipase Cgamma- and RasGRP1-dependent fashion. The specificity of N-Ras signaling downstream of low-grade TCR stimulation was dependent on the monoacylation of the hypervariable membrane targeting sequence. Our data show that, in contrast to fibroblasts stimulated with growth factors in which all three Ras isoforms become activated and signaling occurs at both the plasma membrane and Golgi apparatus, Golgi-associated N-Ras is the critical Ras isoform and intracellular pool for low-grade TCR signaling in Jurkat T cells.

摘要

Ras激活对于T细胞的发育和功能至关重要,但不同Ras亚型在T淋巴细胞功能中的具体作用仍知之甚少。我们最近报道了T细胞受体(TCR)激活了T细胞高尔基体上异位表达的H-Ras。在此,我们研究了Jurkat T细胞中Ras信号的亚型和亚细胞区室特异性。在Jurkat和其他几种T细胞系中,H-Ras的表达水平远低于其他Ras亚型。谷胱甘肽S-转移酶-Ras结合结构域(RBD)下拉试验显示,尽管高强度的TCR刺激和佛波酯激活了N-Ras和K-Ras,但低强度的TCR刺激导致N-Ras的特异性激活。令人惊讶的是,异位表达的H-Ras与TCR在Jurkat质膜的脂质微区中共帽,而N-Ras则不然。对表达绿色荧光蛋白-RBD(一种GTP结合Ras的荧光报告分子)的Jurkat细胞进行活细胞成像显示,N-Ras激活仅以磷脂酶Cγ和RasGRP1依赖的方式在高尔基体上发生。低强度TCR刺激下游N-Ras信号的特异性取决于高变膜靶向序列的单酰化。我们的数据表明,与生长因子刺激的成纤维细胞不同,在成纤维细胞中所有三种Ras亚型均被激活且信号在质膜和高尔基体上均发生,高尔基体相关的N-Ras是Jurkat T细胞中低强度TCR信号的关键Ras亚型和细胞内池。

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