Cas-L的结构与功能,一种105千道尔顿的与Crk相关的底物相关蛋白,参与淋巴细胞中β1整合素介导的信号传导。
Structure and function of Cas-L, a 105-kD Crk-associated substrate-related protein that is involved in beta 1 integrin-mediated signaling in lymphocytes.
作者信息
Minegishi M, Tachibana K, Sato T, Iwata S, Nojima Y, Morimoto C
机构信息
Dana-Farber Cancer Institute, Department of Medicine, Harvard Medical School, Boston, Massachusetts 02115, USA.
出版信息
J Exp Med. 1996 Oct 1;184(4):1365-75. doi: 10.1084/jem.184.4.1365.
Abstract
Integrin/ligand binding evokes tyrosine phosphorylation of various proteins. We reported previously that a 105 kD protein (pp105) was tyrosine phosphorylated by the engagement of beta 1 integrins in T lymphocytes. We show here that pp105 is a novel p130Cas (Crk-associated substrate)-related protein. Deduced amino acid sequence revealed that pp105 contains conserved motifs with p130Cas, and both pp105 and p130Cas bind to focal adhesion kinase (pp125FAK) and Crk. However, pp105 has a clearly distinct structure from p130Cas, and pp105 is preferentially expressed in lymphocytes, whereas p130Cas is expressed in adherent cells. With these findings, we designate pp105 as Cas-L, lymphocyte-type Cas. Furthermore, we demonstrate that integrin/ligand binding results in the recruitment of Crk, Nck, and SHPTP2 to pp105. These findings further define the roles of pp105/Cas-L and pp125FAK in the integrin-mediated signaling pathways.
摘要
整合素/配体结合可引发多种蛋白质的酪氨酸磷酸化。我们先前报道,一种105kD的蛋白质(pp105)在T淋巴细胞中可因β1整合素的结合而发生酪氨酸磷酸化。我们在此表明,pp105是一种新型的与p130Cas(Crk相关底物)相关的蛋白质。推导的氨基酸序列显示,pp105含有与p130Cas保守的基序,并且pp105和p130Cas都与粘着斑激酶(pp125FAK)和Crk结合。然而,pp105与p130Cas具有明显不同的结构,并且pp105在淋巴细胞中优先表达,而p130Cas在贴壁细胞中表达。基于这些发现,我们将pp105命名为Cas-L,即淋巴细胞型Cas。此外,我们证明整合素/配体结合导致Crk、Nck和SHPTP2募集到pp105。这些发现进一步明确了pp105/Cas-L和pp125FAK在整合素介导的信号通路中的作用。
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Structure and function of Cas-L, a 105-kD Crk-associated substrate-related protein that is involved in beta 1 integrin-mediated signaling in lymphocytes.Cas-L的结构与功能,一种105千道尔顿的与Crk相关的底物相关蛋白,参与淋巴细胞中β1整合素介导的信号传导。
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