首页> 外文会议>PSB;Pacific symposium on biocomputing; 20090105-09;20090105-09; Kohala Coast, HI(US);Kohala Coast, HI(US) >DISSECTING THE INTERFACE BETWEEN SIGNALING AND TRANSCRIPTIONAL REGULATION IN HUMAN B CELLS
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DISSECTING THE INTERFACE BETWEEN SIGNALING AND TRANSCRIPTIONAL REGULATION IN HUMAN B CELLS

机译:剖析人类B细胞的信号传递和转录调控之间的界面

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A key role of signal transduction pathways is to control transcriptional programs in the nucleus as a function of signals received by the cell via complex post-translational modification cascades. This determines cell-context specific responses to environmental stimuli. Given the difficulty of quantitating protein concentration and post-translational modifications, signaling pathway studies are still for the most part conducted one interaction at the time. Thus, genome-wide, cell-context specific dissection of signaling pathways is still an open challenge in molecular systems biology. In this manuscript we extend the MINDy algorithm for the identification of post-translational modulators of transcription factor activity, to produce a first genome-wide map of the interface between signaling and transcriptional regulatory programs in human b cells. We show that the serine-threonine kinase STK38 emerges as the most pleiotropic signaling protein in this cellular context and we biochemically validate this finding by shRNA-mediated silencing of this kinase, followed by gene expression profile analysis. We also extensively validate the inferred interactions using protein-protein interaction databases and the kinase-substrate interaction prediction algorithm NetworKIN.
机译:信号转导途径的关键作用是控制细胞核中的转录程序,作为细胞通过复杂的翻译后修饰级联反应所接收信号的函数。这确定了对环境刺激的细胞背景特异性反应。考虑到定量蛋白质浓度和翻译后修饰的困难,当时大多数情况下,信号通路研究仍只进行一种相互作用。因此,信号通路的全基因组,细胞背景特异性解剖仍然是分子系统生物学中的一个开放挑战。在本手稿中,我们扩展了MINDy算法,以识别转录因子活性的翻译后调节剂,以生成人b细胞中信号传导和转录调控程序之间接口的第一个全基因组图。我们显示丝氨酸-苏氨酸激酶STK38出现在这种细胞环境中最多效性信号蛋白,我们通过shRNA介导的该激酶的沉默,然后进行基因表达谱分析,通过生物化学方法验证了这一发现。我们还使用蛋白质-蛋白质相互作用数据库和激酶-底物相互作用预测算法NetworKIN广泛验证了推断的相互作用。

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