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Inhibition of beta 2 integrin receptor and Syk kinase signaling in monocytes by the Src family kinase Fgr.

机译:Src家族激酶Fgr对单核细胞中β2整合素受体和Syk激酶信号的抑制作用。

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摘要

While beta 2 integrin ligand-receptor recognition interactions are well characterized, less is known about how these events trigger signal transduction cascades to regulate the transition from tethering to firm adhesion, spreading, and transendothelial migration. We have identified critical positive and negative regulatory components of this cascade in monocytes. Whereas the Syk tyrosine kinase is essential for beta 2 integrin signaling and cell spreading, the Src family kinase Fgr is a negative regulator of this pathway. Fgr selectively inhibits beta 2 but not beta 1 integrin signaling and Syk kinase function via a direct association between the Fgr SH2 domain and Syk tyrosine Y342. The inhibitory effects of Fgr are independent of its kinase activity, are dose dependent, and can be overcome by chemokines and inflammatory mediators.
机译:尽管已经很好地描述了β2整联蛋白配体-受体识别相互作用,但对于这些事件如何触发信号转导级联反应以调节从束缚到牢固粘附,扩散和跨内皮迁移的转变知之甚少。我们已经确定了单核细胞中该级联反应的关键的正负调节成分。 Syk酪氨酸激酶对于β2整联蛋白信号传导和细胞扩散至关重要,而Src家族激酶Fgr是该途径的负调控因子。 Fgr通过Fgr SH2域和Syk酪氨酸Y342之间的直接关联,选择性抑制beta 2但不抑制beta 1整合素信号传导和Syk激酶功能。 Fgr的抑制作用与其激酶活性无关,是剂量依赖性的,可以被趋化因子和炎性介质克服。

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