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PRYSPRY介导的三聚体基序(TRIM)蛋白功能的结构基础。

Structural basis for PRYSPRY-mediated tripartite motif (TRIM) protein function.

作者信息

James Leo C, Keeble Anthony H, Khan Zahra, Rhodes David A, Trowsdale John

机构信息

Protein and Nucleic Acid Chemistry Division, Medical Research Council Laboratory of Molecular Biology, Cambridge CB2 2QH, UK.

出版信息

Proc Natl Acad Sci U S A. 2007 Apr 10;104(15):6200-5. doi: 10.1073/pnas.0609174104. Epub 2007 Mar 30.

Abstract

The human tripartite motif (TRIM) family comprises 70 members, including HIV restriction factor TRIM5alpha and disease-associated proteins TRIM20 (pyrin) and TRIM21. TRIM proteins have conserved domain architecture but diverse cellular roles. Here, we describe how the C-terminal PRYSPRY domain mediates diverse TRIM functions. The crystal structure of TRIM21 PRYSPRY in complex with its target IgG Fc reveals a canonical binding interface comprised of two discrete pockets formed by antibody-like variable loops. Alanine scanning of this interface has identified the hot-spot residues that control TRIM21 binding to Fc; the same hot-spots control HIV/murine leukemia virus restriction by TRIM5alpha and mediate severe familial Mediterranean fever in TRIM20/pyrin. Characterization of the IgG binding site for TRIM21 PRYSPRY reveals TRIM21 as a superantigen analogous to bacterial protein A and suggests that an antibody bipolar bridging mechanism may contribute to the pathogenic accumulation of anti-TRIM21 autoantibody immune complex in autoimmune disease.

摘要

人类三联基序(TRIM)家族由70个成员组成,包括HIV限制因子TRIM5α以及与疾病相关的蛋白TRIM20(吡啉)和TRIM21。TRIM蛋白具有保守的结构域架构,但在细胞中发挥着多样的作用。在此,我们描述了C端PRYSPRY结构域如何介导TRIM的多种功能。TRIM21的PRYSPRY结构域与其靶标IgG Fc形成复合物的晶体结构揭示了一个典型的结合界面,该界面由抗体样可变环形成的两个离散口袋组成。对该界面进行丙氨酸扫描已确定了控制TRIM21与Fc结合的热点残基;相同的热点控制TRIM5α对HIV/小鼠白血病病毒的限制,并在TRIM20/吡啉中引发严重的家族性地中海热。对TRIM21的PRYSPRY结构域IgG结合位点的表征揭示TRIM21是一种类似于细菌蛋白A的超抗原,并表明抗体双极桥接机制可能导致自身免疫疾病中抗TRIM21自身抗体免疫复合物的致病性积累。

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Structural basis for PRYSPRY-mediated tripartite motif (TRIM) protein function.PRYSPRY介导的三聚体基序(TRIM)蛋白功能的结构基础。
Proc Natl Acad Sci U S A. 2007 Apr 10;104(15):6200-5. doi: 10.1073/pnas.0609174104. Epub 2007 Mar 30.

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