肝细胞生长因子刺激细胞分散需要 ERK 和 Cdc42 依赖性紧密连接解体。
Hepatocyte Growth Factor stimulated cell scattering requires ERK and Cdc42-dependent tight junction disassembly.
机构信息
Section of Nephrology, Yale University School of Medicine, New Haven, CT 06520, USA.
出版信息
Biochem Biophys Res Commun. 2010 Sep 17;400(2):271-7. doi: 10.1016/j.bbrc.2010.08.060. Epub 2010 Aug 20.
Abstract
The mechanism by which Hepatocyte Growth Factor (HGF) induces tight junction disassembly prior to cell scattering is largely unknown. Here, we show that HGF stimulates rapid loss of the TJ assembly protein Par6 from the TJ in an Erk-dependent manner. Erk activation by HGF is found to mediate the interaction of Par6 with GTP-loaded Cdc42. The Cdc42 GTPase activating protein cdGAP is shown to interact with Pkcζ at baseline and prevent Par6-Cdc42 association. Erk, by phosphorylating cdGAP at threonine776, can inhibit the GAP activity, thereby increasing Par6-Cdc42 association and TJ disassembly. Our findings reveal a novel pathway for regulating HGF signaling to the Par proteins through Erk-cdGAP, resulting in TJ disassembly and cell scattering.
摘要
肝细胞生长因子(HGF)在细胞分散之前诱导紧密连接解体的机制在很大程度上是未知的。在这里,我们表明 HGF 以依赖 Erk 的方式刺激 TJ 组装蛋白 Par6 从 TJ 中的快速丢失。发现 HGF 对 Erk 的激活介导了 Par6 与 GTP 加载的 Cdc42 的相互作用。Cdc42 GTPase 激活蛋白 cdGAP 被显示在基线时与 Pkcζ相互作用,并防止 Par6-Cdc42 缔合。Erk 通过 Thr776 磷酸化 cdGAP,可以抑制 GAP 活性,从而增加 Par6-Cdc42 缔合和 TJ 解体。我们的发现揭示了一种通过 Erk-cdGAP 调节 HGF 信号向 Par 蛋白的新途径,导致 TJ 解体和细胞分散。
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