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The PTB domain of ShcA couples receptor activation to the cytoskeletal regulator IQGAP1

机译:ShcA的PTB结构域将受体激活与细胞骨架调节剂IQGAP1耦合

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摘要

Adaptor proteins respond to stimuli and recruit downstream complexes using interactions conferred by associated protein domains and linear motifs. The ShcA adaptor contains two phosphotyrosine recognition modules responsible for binding activated receptors, resulting in the subsequent recruitment of Grb2 and activation of Ras/MAPK. However, there is evidence that Grb2-independent signalling from ShcA has an important role in development. Using mass spectrometry, we identified the multidomain scaffold IQGAP1 as a ShcA-interacting protein. IQGAP1 and ShcA co-precipitate and are co-recruited to membrane ruffles induced by activated receptors of the ErbB family, and a reduction in ShcA protein levels inhibits the formation of lamellipodia. We used NMR to characterize a direct, non-canonical ShcA PTB domain interaction with a helical fragment from the IQGAP1 N-terminal region that is pTyr-independent. This interaction is mutually exclusive with binding to a more conventional PTB domain peptide ligand from PTP–PEST. ShcA-mediated recruitment of IQGAP1 may have an important role in cytoskeletal reorganization downstream of activated receptors at the cell surface.
机译:衔接蛋白利用相关的蛋白质结构域和线性基序赋予的相互作用,对刺激作出反应并募集下游复合物。 ShcA衔接子包含两个磷酸酪氨酸识别模块,负责结合激活的受体,导致随后募集Grb2和激活Ras / MAPK。但是,有证据表明,ShcA的不依赖Grb2的信号在发育中具有重要作用。使用质谱,我们确定了多域支架IQGAP1作为ShcA相互作用蛋白。 IQGAP1和ShcA共同沉淀,并共同招募到ErbB家族的活化受体诱导的膜褶皱上,ShcA蛋白水平的降低会抑制片状脂蛋白的形成。我们使用NMR来表征与来自IQTAP1 N末端区域的螺旋片段(与pTyr无关)的直接,非规范ShcA PTB域相互作用。这种相互作用与PTP–PEST中更常规的PTB域肽配体的结合相互排斥。 ShcA介导的IQGAP1募集可能在细胞表面活化受体下游的细胞骨架重组中起重要作用。

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