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FES 激酶参与 KIT 配体诱导的趋化作用。

FES kinase participates in KIT-ligand induced chemotaxis.

机构信息

INSERM U891, Centre de Recherche en Cancérologie de Marseille (CRCM), Marseille, France.

出版信息

Biochem Biophys Res Commun. 2010 Feb 26;393(1):174-8. doi: 10.1016/j.bbrc.2010.01.116. Epub 2010 Feb 1.

DOI:10.1016/j.bbrc.2010.01.116
PMID:20117079
Abstract

FES is a cytoplasmic tyrosine kinase activated by several membrane receptors, originally identified as a viral oncogene product. We have recently identified FES as a crucial effector of oncogenic KIT mutant receptor. However, FES implication in wild-type KIT receptor function was not addressed. We report here that FES interacts with KIT and is phosphorylated following activation by its ligand SCF. Unlike in the context of oncogenic KIT mutant, FES is not involved in wild-type KIT proliferation signal, or in cell adhesion. Instead, FES is required for SCF-induced chemotaxis. In conclusion, FES kinase is a mediator of wild-type KIT signalling implicated in cell migration.

摘要

FES 是一种细胞质酪氨酸激酶,可被几种膜受体激活,最初被鉴定为一种病毒癌基因产物。我们最近发现 FES 是致癌 KIT 突变受体的关键效应物。然而,FES 在野生型 KIT 受体功能中的作用尚未得到解决。我们在这里报告,FES 与 KIT 相互作用,并在其配体 SCF 激活后被磷酸化。与致癌 KIT 突变的情况不同,FES 不参与野生型 KIT 增殖信号或细胞黏附。相反,FES 是 SCF 诱导的趋化作用所必需的。总之,FES 激酶是参与细胞迁移的野生型 KIT 信号转导的介质。

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