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人源蛋白酪氨酸磷酸酶 SHP-1 开放构象的晶体结构。

Crystal structure of human protein tyrosine phosphatase SHP-1 in the open conformation.

机构信息

Department of Biological Sciences, Louisiana State University, Baton Rouge, Louisiana 70803, USA.

出版信息

J Cell Biochem. 2011 Aug;112(8):2062-71. doi: 10.1002/jcb.23125.

Abstract

SHP-1 belongs to the family of non-receptor protein tyrosine phosphatases (PTPs) and generally acts as a negative regulator in a variety of cellular signaling pathways. Previously, the crystal structures of the tail-truncated SHP-1 and SHP-2 revealed an autoinhibitory conformation. To understand the regulatory mechanism of SHP-1, we have determined the crystal structure of the full-length SHP-1 at 3.1 Å. Although the tail was disordered in current structure, the huge conformational rearrangement of the N-SH2 domain and the incorporation of sulfate ions into the ligand-binding site of each domain indicate that the SHP-1 is in the open conformation. The N-SH2 domain in current structure is shifted away from the active site of the PTP domain to the other side of the C-SH2 domain, resulting in exposure of the active site. Meanwhile, the C-SH2 domain is twisted anticlockwise by about 110°. In addition, a set of new interactions between two SH2 domains and between the N-SH2 and the catalytic domains is identified, which could be responsible for the stabilization of SHP-1 in the open conformation. Based on the structural comparison, a model for the activation of SHP-1 is proposed.

摘要

SHP-1 属于非受体酪氨酸磷酸酶(PTPs)家族,通常在多种细胞信号通路中充当负调节剂。先前,截短的 SHP-1 和 SHP-2 的晶体结构揭示了一种自动抑制构象。为了了解 SHP-1 的调节机制,我们已经确定了全长 SHP-1 在 3.1Å 的晶体结构。尽管当前结构中的尾部是无序的,但 N-SH2 结构域的巨大构象重排以及每个结构域的配体结合位点中硫酸盐离子的掺入表明 SHP-1 处于开放构象。当前结构中的 N-SH2 结构域从 PTP 结构域的活性位点移到 C-SH2 结构域的另一侧,导致活性位点暴露。同时,C-SH2 结构域逆时针扭转约 110°。此外,还确定了一组新的 SH2 结构域之间以及 N-SH2 和催化结构域之间的相互作用,这可能是 SHP-1 稳定在开放构象中的原因。基于结构比较,提出了 SHP-1 激活的模型。

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