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Divergent Roles of c-Src in Controlling Platelet-derived Growth Factor-dependent Signaling in FibroblastsD⃞

机译:c-Src在控制成纤维细胞中血小板衍生的生长因子依赖性信号传导中的不同作用

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摘要

The vast complexity of platelet-derived growth factor (PDGF)-induced downstream signaling pathways is well known, but the precise roles of critical players still elude us due to our lack of specific and temporal control over their activities. Accordingly, although Src family members are some of the better characterized effectors of PDGFβ signaling, considerable controversy still surrounds their precise functions. To address these questions and limitations, we applied a chemical–genetic approach to study the role of c-Src at the cellular level, in defined signaling cascades; we also uncovered novel phosphorylation targets and defined its influence on transcriptional events. The spectacular control of c-Src on actin reorganization and chemotaxis was delineated by global substrate labeling and transcriptional analysis, revealing multiple cytoskeletal proteins and chemotaxis promoting genes to be under c-Src control. Additionally, this tool revealed the contrasting roles of c-Src in controlling DNA synthesis, where it transmits conflicting inputs via the phosphatidylinositol 3 kinase and Ras pathways. Finally, this study reveals a mechanism by which Src family kinases may control PDGF-mediated responses both at transcriptional and translational levels.
机译:血小板衍生的生长因子(PDGF)诱导的下游信号通路的巨大复杂性是众所周知的,但是由于我们缺乏对其活动的特异性和时间控制,关键角色的确切角色仍然使我们难以捉摸。因此,尽管Src家族成员是PDGFβ信号转导的一些更好表征的效应物,但是其精确功能仍存在相当大的争议。为了解决这些问题和局限性,我们应用化学-遗传方法研究了c-Src在细胞水平上在定义的信号级联反应中的作用。我们还发现了新型的磷酸化目标,并定义了其对转录事件的影响。通过全局底物标记和转录分析描绘了c-Src对肌动蛋白重组和趋化性的惊人控制,揭示了多个细胞骨架蛋白和趋化性促进基因处于c-Src的控制之下。此外,该工具揭示了c-Src在控制DNA合成中的不同作用,在该过程中,它通过磷脂酰肌醇3激酶和Ras途径传输有冲突的输入。最后,这项研究揭示了Src家族激酶可以在转录和翻译水平上控制PDGF介导的反应的机制。

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