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对B30.2/SPRY结构域的结构与功能见解

Structural and functional insights into the B30.2/SPRY domain.

作者信息

Woo Jae-Sung, Imm Joon-Hyuk, Min Chang-Ki, Kim Kyung-Jin, Cha Sun-Shin, Oh Byung-Ha

机构信息

Division of Molecular and Life Sciences, Department of Life Sciences, Center for Biomolecular Recognition, Pohang University of Science and Technology, Pohang, Kyungbuk, Korea.

出版信息

EMBO J. 2006 Mar 22;25(6):1353-63. doi: 10.1038/sj.emboj.7600994. Epub 2006 Feb 23.

Abstract

The B30.2/SPRY domain is present in approximately 700 eukaryotic (approximately 150 human) proteins, including medically important proteins such as TRIM5alpha and Pyrin. Nonetheless, the functional role of this modular domain remained unclear. Here, we report the crystal structure of an SPRY-SOCS box family protein GUSTAVUS in complex with Elongins B and C, revealing a highly distorted two-layered beta-sandwich core structure of its B30.2/SPRY domain. Ensuing studies identified one end of the beta-sandwich as the surface interacting with an RNA helicase VASA with a 40 nM dissociation constant. The sequence variation in TRIM5alpha responsible for HIV-1 restriction and most of the mutations in Pyrin causing familial Mediterranean fever map on this surface, implicating the corresponding region in many B30.2/SPRY domains as the ligand-binding site. The amino acids lining the binding surface are highly variable among the B30.2/SPRY domains, suggesting that these domains are protein-interacting modules, which recognize a specific individual partner protein rather than a consensus sequence motif.

摘要

B30.2/SPRY结构域存在于大约700种真核生物(约150种人类)蛋白质中,包括医学上重要的蛋白质,如TRIM5α和吡啉。尽管如此,这个模块化结构域的功能作用仍不清楚。在这里,我们报告了一种SPRY-SOCS盒家族蛋白古斯塔夫斯(GUSTAVUS)与延伸蛋白B和C复合物的晶体结构,揭示了其B30.2/SPRY结构域高度扭曲的两层β折叠三明治核心结构。随后的研究确定β折叠三明治的一端是与RNA解旋酶VASA相互作用的表面,解离常数为40 nM。负责HIV-1限制的TRIM5α中的序列变异以及导致家族性地中海热的吡啉中的大多数突变都定位在这个表面上,这表明许多B30.2/SPRY结构域中的相应区域是配体结合位点。在B30.2/SPRY结构域中,结合表面的氨基酸高度可变,这表明这些结构域是蛋白质相互作用模块,识别特定的单个伴侣蛋白而不是共有序列基序。

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