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RhoG regulates gene expression and the actin cytoskeleton in lymphocytes

机译:RhoG调节淋巴细胞中的基因表达和肌动蛋白细胞骨架

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摘要

RhoG, a member of the Rho family of GTPases, has been implicated as a regulator of the actin cytoskeleton. In this study, we show a novel function for the small GTPase RhoG on the regulation of the interferon- promoter and nuclear factor of activated T cells (NFAT) gene transcription in lymphocytes. Optimal function of RhoG for the expression of these genes requires a calcium signal, normally provided by the antigen receptor. In addition, RhoG potentiation of NFAT requires the indirect activity of Rac and Cdc42; however, pathways distinct from those activated by Rac and Cdc42 mediate RhoG activation of NFAT-dependent transcription. Using effector domain mutants of RhoG we found that its ability to potentiate NFAT-dependent transcription correlates with its capacity to increase actin polymerization, supporting the suggestion that NFAT-dependent transcription is an actin-dependent process. RhoG also promotes T-cell spreading on fibronectin, a property that is independent of its ability to enhance NFAT-dependent transcription. Hence, these results implicate RhoG in leukocyte trafficking and the control of gene expression induced in response to antigen encounter.
机译:RhoG是GTPases Rho家族的成员,已被认为是肌动蛋白细胞骨架的调节剂。在这项研究中,我们显示了小GTPase RhoG在调节淋巴细胞中干扰素启动子和活化T细胞(NFAT)基因转录的核因子方面的新功能。 RhoG对这些基因表达的最佳功能需要钙信号,通常由抗原受体提供。另外,NFAT的RhoG增强需要Rac和Cdc42的间接活性。但是,与Rac和Cdc42激活的途径不同的途径介导了NFAT依赖性转录的RhoG激活。使用RhoG的效应子域突变体,我们发现其增强NFAT依赖性转录的能力与其增加肌动蛋白聚合的能力相关,支持NFAT依赖性转录是肌动蛋白依赖性过程的提示。 RhoG还促进T细胞在纤连蛋白上扩散,这一特性与其增强NFAT依赖性转录的能力无关。因此,这些结果暗示RhoG参与白细胞运输和响应于抗原遭遇而诱导的基因表达的控制。

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