首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Signaling Scaffold Protein IQGAP1 Interacts with Microtubule Plus-end Tracking Protein SKAP and Links Dynamic Microtubule Plus-end to Steer Cell Migration
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Signaling Scaffold Protein IQGAP1 Interacts with Microtubule Plus-end Tracking Protein SKAP and Links Dynamic Microtubule Plus-end to Steer Cell Migration

机译:信号支架蛋白IQGAP1与微管+末端跟踪蛋白SKAP相互作用,并将动态微管+末端链接到引导细胞迁移

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摘要

Cell migration is orchestrated by dynamic interaction of microtubules with the plasma membrane cortex. However, the regulatory mechanisms underlying the cortical actin cytoskeleton and microtubule dynamics are less characterized. Our earlier study showed that small GTPase-activating proteins, IQGAPs, regulate polarized secretion in epithelial cells (). Here, we show that IQGAP1 links dynamic microtubules to steer cell migration via interacting with the plus-end tracking protein, SKAP. Biochemical characterizations revealed that IQGAP1 and SKAP form a cognate complex and that their binding interfaces map to the WWIQ motif and the C-terminal of SKAP, respectively. The WWIQ peptide disrupts the biochemical interaction between IQGAP1 and SKAP in vitro, and perturbation of the IQGAP1-SKAP interaction in vivo using a membrane-permeable TAT-WWIQ peptide results in inhibition of directional cell migration elicited by EGF. Mechanistically, the N-terminal of SKAP binds to EB1, and its C terminus binds to IQGAP1 in migrating cells. Thus, we reason that a novel IQGAP1 complex orchestrates directional cell migration via coupling dynamic microtubule plus-ends to the cell cortex.
机译:细胞迁移是通过微管与质膜皮质的动态相互作用来进行的。但是,皮质肌动蛋白的细胞骨架和微管动力学的潜在调控机制较少。我们较早的研究表明,小的GTPase激活蛋白IQGAP调节上皮细胞的极化分泌()。在这里,我们表明IQGAP1通过与正向追踪蛋白SKAP相互作用,将动态微管链接到引导细胞迁移。生化特征表明,IQGAP1和SKAP形成同源复合物,它们的结合界面分别映射到WWIQ基序和SKAP的C末端。 WWIQ肽在体外破坏了IQGAP1和SKAP之间的生化相互作用,使用膜透性TAT-WWIQ肽在体内扰动IQGAP1-SKAP相互作用导致抑制了EGF诱导的定向细胞迁移。从机理上讲,在迁移细胞中,SKAP的N末端与EB1结合,其C末端与IQGAP1结合。因此,我们认为一种新型的IQGAP1复合物通过将动态微管正向末端耦合到细胞皮层来协调定向细胞的迁移。

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