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粘着斑激酶:处于信号转导的十字路口

Focal adhesion kinase: at the crossroads of signal transduction.

作者信息

Ilić D, Damsky C H, Yamamoto T

机构信息

Department of Oncology, Institute of Medical Science, Tokyo University, Minato-ku, Japan.

出版信息

J Cell Sci. 1997 Feb;110 ( Pt 4):401-7. doi: 10.1242/jcs.110.4.401.

Abstract

Morphogenetic processes during development, including cell migration, depend on signals from both the extracellular matrix (ECM) and soluble signaling factors. Extensive evidence has shown that the nonreceptor tyrosine kinase, focal adhesion kinase (FAK), is activated in response to both kind of signal. The most definitive evidence that FAK is directly downstream of signals initiated by the ECM comes from comparing the phenotypes of mice deficient for FAK and the ECM molecule, fibronectin: in both cases embryos die at about E8.5 and display almost identical severe vascular and other mesodermal defects. It is now clear that there are additional FAK-like proteins, indicating the existence of a FAK family. Furthermore, FAK is not located at adhesive sites in all cells where it is expressed. This, plus extensive data indicating that FAK becomes activated in response to several soluble signaling factors, suggests that the FAK family may be at the crossroads of multiple signaling pathways that affect cell and developmental processes.

摘要

发育过程中的形态发生过程,包括细胞迁移,依赖于细胞外基质(ECM)和可溶性信号因子发出的信号。大量证据表明,非受体酪氨酸激酶——粘着斑激酶(FAK),会对这两种信号作出反应而被激活。FAK直接位于由ECM引发的信号下游,这一最确凿的证据来自于对缺乏FAK的小鼠和ECM分子纤连蛋白的小鼠表型进行比较:在这两种情况下,胚胎大约在胚胎期8.5天死亡,并表现出几乎相同的严重血管和其他中胚层缺陷。现在很清楚,存在其他FAK样蛋白,这表明存在一个FAK家族。此外,FAK并不位于其所有表达细胞的粘附位点。这一点,再加上大量数据表明FAK会对多种可溶性信号因子作出反应而被激活,表明FAK家族可能处于影响细胞和发育过程的多条信号通路的交叉点上。

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