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脑特异性衔接蛋白ShcC的磷酸酪氨酸结合结构域的结合特异性及突变分析

Binding specificity and mutational analysis of the phosphotyrosine binding domain of the brain-specific adaptor protein ShcC.

作者信息

O'Bryan J P, Martin C B, Songyang Z, Cantley L C, Der C J

机构信息

Department of Pharmacology, University of North Carolina, Chapel Hill 27599, USA.

出版信息

J Biol Chem. 1996 May 17;271(20):11787-91. doi: 10.1074/jbc.271.20.11787.

Abstract

Shc proteins (hereafter referred to as ShcA) represent major substrates of tyrosine phosphorylation by a wide variety of growth factors and cytokines. We have recently described a novel ShcA-like protein, ShcC, which like ShcA contains an NH2-terminal phosphotyrosine binding domain (PTB), a central effector region (CH1) and a COOH-terminal Src homology 2 domain (SH2). Both the SH2 and PTB domains of ShcC bind a similar profile of proteins as the comparable regions of ShcA. In an effort to define the functional differences or similarities between ShcA and ShcC, we have further characterized the PTB domain of ShcC. Using a degenerate phosphopeptide library screen, we show that the PTB domain of ShcC preferentially binds the sequence His-hydrophobic-Asn/hydrophobic-Asn-Pro-Ser/Thr-Tyr(P). This sequence is similar to the binding site for the ShcA PTB domain, suggesting that these two proteins may have overlapping specificities. In addition, random mutagenesis of the ShcC PTB domain has identified several amino acids important for PTB function (Gly32, Glu63, Ala136, Gly139, and Asp140). Mutation of these amino acids dramatically reduces the affinity of the ShcC PTB domain for the activated epidermal growth factor receptor in vitro.

摘要

Shc蛋白(以下简称ShcA)是多种生长因子和细胞因子酪氨酸磷酸化的主要底物。我们最近描述了一种新型的ShcA样蛋白ShcC,它与ShcA一样,含有一个NH2末端的磷酸酪氨酸结合结构域(PTB)、一个中央效应区域(CH1)和一个COOH末端的Src同源2结构域(SH2)。ShcC的SH2和PTB结构域与ShcA的相应区域结合的蛋白质谱相似。为了确定ShcA和ShcC之间的功能差异或相似性,我们进一步对ShcC的PTB结构域进行了表征。通过使用简并磷酸肽文库筛选,我们发现ShcC的PTB结构域优先结合序列His-疏水-Asn/疏水-Asn-Pro-Ser/Thr-Tyr(P)。该序列与ShcA PTB结构域的结合位点相似,表明这两种蛋白质可能具有重叠的特异性。此外,对ShcC PTB结构域的随机诱变确定了几个对PTB功能重要的氨基酸(Gly32、Glu63、Ala136、Gly139和Asp140)。这些氨基酸的突变在体外显著降低了ShcC PTB结构域对活化表皮生长因子受体的亲和力。

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