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Identification of Novel Focal Adhesion Kinase Substrates: Role for FAK in NFκB Signaling

机译:新型局灶性粘附激酶底物的鉴定:FAK在NFκB信号传导中的作用

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摘要

Focal adhesion kinase (FAK) is a major signaling molecule which functions downstream of integrins or in conjunction with mitogenic signaling pathways. FAK is overexpressed and/or activated in many types of human tumors, in which it promotes cell adhesion, survival, migration and invasion. In addition to FAK's ability to regulate signaling through its scaffolding activities, FAK encodes an intrinsic kinase activity. Although some FAK substrates have been identified, a more comprehensive analysis of substrates is lacking. In this study, we use a protein microarray to screen the human proteome for FAK substrates. We confirm that several of the proteins identified are bona fide in vitro FAK substrates, including several factors which are known to regulate the NFκB pathway. Finally, we identify a role for FAK's kinase activity in both canonical and non-canonical NFκB signaling. Our screen therefore represents the first high throughput screen for FAK substrates and provides the basis for future in-depth analysis of the role of FAK's kinase activity in the processes of tumorigenesis.
机译:黏着斑激酶(FAK)是主要的信号分子,在整联蛋白的下游或与促有丝分裂的信号通路一起起作用。 FAK在许多类型的人类肿瘤中过表达和/或活化,在其中它促进细胞粘附,存活,迁移和侵袭。 FAK除了通过其支架活动调节信号传导的能力外,还可以编码内在的激酶活性。尽管已识别出一些FAK底物,但缺乏对底物的更全面分析。在这项研究中,我们使用蛋白质微阵列来筛选人类蛋白质组中FAK底物。我们确认,鉴定出的几种蛋白质是真正的体外FAK底物,包括已知调节NFκB途径的几种因素。最后,我们确定了FAK激酶活性在规范和非规范NFκB信号传导中的作用。因此,我们的筛选代表了FAK底物的首个高通量筛选,并为将来深入分析FAK激酶活性在肿瘤发生过程中的作用提供了基础。

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