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Functional Proteomics Mapping of a Human Signaling Pathway

机译:人类信号通路的功能蛋白质组学映射

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摘要

Access to the human genome facilitates extensive functional proteomics studies. Here, we present an integrated approach combining large-scale protein interaction mapping, exploration of the interaction network, and cellular functional assays performed on newly identified proteins involved in a human signaling pathway. As a proof of principle, we studied the Smad signaling system, which is regulated by members of the transforming growth factor β (TGFβ) superfamily. We used two-hybrid screening to map Smad signaling protein–protein interactions and to establish a network of 755 interactions, involving 591 proteins, 179 of which were poorly or not annotated. The exploration of such complex interaction databases is improved by the use of PIMRider, a dedicated navigation tool accessible through the Web. The biological meaning of this network is illustrated by the presence of 18 known Smad-associated proteins. Functional assays performed in mammalian cells including siRNA knock-down experiments identified eight novel proteins involved in Smad signaling, thus validating this integrated functional proteomics approach.
机译:进入人类基因组有助于广泛的功能蛋白质组学研究。在这里,我们提出了一种整合的方法,该方法结合了大规模蛋白质相互作用图谱,相互作用网络的探索以及对人信号传导途径中新近鉴定出的蛋白质进行的细胞功能测定。作为原理的证明,我们研究了Smad信号系统,该系统受转化生长因子β(TGFβ)超家族成员的调节。我们使用两次杂交筛选来绘制Smad信号蛋白与蛋白的相互作用图,并建立755个相互作用的网络,其中涉及591个蛋白,其中179个蛋白标记不佳或未加注释。通过使用PIMRider(一种可通过Web访问的专用导航工具),改进了对此类复杂交互数据库的探索。该网络的生物学意义通过存在18种已知的Smad相关蛋白来说明。在哺乳动物细胞中进行的功能分析(包括siRNA敲低实验)确定了8种与Smad信号传导有关的新型蛋白质,从而验证了这种集成的功能蛋白质组学方法。

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