Zakaria Shaheen, Gomez Timothy S, Savoy Doris N, McAdam Simon, Turner Martin, Abraham Robert T, Billadeau Daniel D
Division of Oncology Research, Mayo Clinic College of Medicine, Rochester, MN 55905, USA.
J Exp Med. 2004 Feb 2;199(3):429-34. doi: 10.1084/jem.20031228.
Although all three Vav family members are expressed in T lymphocytes, the role that Vav3 plays in T cell activation is poorly defined. Here we show that, like Vav1, Vav3 undergoes rapid tyrosine phosphorylation after T cell receptor (TCR) cross-linkage and interacts with the adaptor molecules SLP76 and 3BP2 in a SH2-dependent manner. However, depletion of Vav1 but not Vav3 protein by RNA interference affects TCR-mediated IL-2 promoter activity. In contrast, Vav3 function is specifically required for coupling TCR stimulation to serum response element-mediated gene transcription. These data indicate that, although both Vav proteins are biochemically coupled to the TCR, they regulate distinct molecular pathways leading to defined gene transcriptional events.
尽管Vav家族的所有三个成员都在T淋巴细胞中表达,但Vav3在T细胞激活中所起的作用仍不清楚。我们在此表明,与Vav1一样,Vav3在T细胞受体(TCR)交联后会迅速发生酪氨酸磷酸化,并以SH2依赖性方式与衔接分子SLP76和3BP2相互作用。然而,通过RNA干扰耗尽Vav1而非Vav3蛋白会影响TCR介导的IL-2启动子活性。相反,将TCR刺激与血清反应元件介导的基因转录偶联特别需要Vav3的功能。这些数据表明,尽管两种Vav蛋白在生化上都与TCR偶联,但它们调节导致特定基因转录事件的不同分子途径。
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