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磷酸酶SH-PTP2的串联SH2结构域对磷酸化蛋白识别的空间限制

Spatial constraints on the recognition of phosphoproteins by the tandem SH2 domains of the phosphatase SH-PTP2.

作者信息

Eck M J, Pluskey S, Trüb T, Harrison S C, Shoelson S E

机构信息

Laboratory of Molecular Medicine, Children's Hospital, Boston, Massachusetts, USA.

出版信息

Nature. 1996 Jan 18;379(6562):277-80. doi: 10.1038/379277a0.

Abstract

The domain organization of many signalling proteins facilitates a segregation of binding, catalytic and regulatory functions. The mammalian SH2 domain protein tyrosine phosphatases (PTPs) contain tandem SH2 domains and a single carboxy-terminal catalytic domain. SH-PTP1 (PTP1C, HCP) and SH-PTP2 (Syp, PTP2C, PTP1D) function downstream from tyrosine kinase-linked insulin, growth factor, cytokine and antigen receptors. As well as directing subcellular localization by binding to receptors and their substrates, the two SH2 domains of these PTPs function together to regulate catalysis. Here we report the structure of the tandem SH2 domains of SH-PTP2 in complex with monophosphopeptides. A fixed relative orientation of the two domains, stabilized by a disulphide bond and a small hydrophobic patch within the interface, separates the peptide binding sites by approximately 40 A. The defined orientation of the SH2 domains in the structure, and data showing that peptide orientation and spacing between binding sites is critical for enzymatic activation, suggest that spatial constraints are important in this multidomain protein-protein interaction.

摘要

许多信号蛋白的结构域组织有助于结合、催化和调节功能的分离。哺乳动物的SH2结构域蛋白酪氨酸磷酸酶(PTP)包含串联的SH2结构域和一个单一的羧基末端催化结构域。SH-PTP1(PTP1C,HCP)和SH-PTP2(Syp,PTP2C,PTP1D)在酪氨酸激酶连接的胰岛素、生长因子、细胞因子和抗原受体的下游发挥作用。除了通过与受体及其底物结合来指导亚细胞定位外,这些PTP的两个SH2结构域共同发挥作用来调节催化作用。在此,我们报道了与单磷酸肽结合的SH-PTP2串联SH2结构域的结构。两个结构域通过二硫键和界面内的一个小疏水区域稳定的固定相对取向,使肽结合位点相隔约40埃。结构中SH2结构域的确定取向,以及表明肽的取向和结合位点之间的间距对酶激活至关重要的数据,表明空间限制在这种多结构域蛋白质-蛋白质相互作用中很重要。

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