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变形链球菌抗原 I/II C 末端区域的晶体结构及唾液黏附素结合域的特性分析。

Crystal structure of the C-terminal region of Streptococcus mutans antigen I/II and characterization of salivary agglutinin adherence domains.

机构信息

Department of Physiology and Biophysics, University of Alabama, Birmingham, Alabama 35294, USA.

出版信息

J Biol Chem. 2011 Jun 17;286(24):21657-66. doi: 10.1074/jbc.M111.231100. Epub 2011 Apr 19.

Abstract

The Streptococcus mutans antigen I/II (AgI/II) is a cell surface-localized protein that adheres to salivary components and extracellular matrix molecules. Here we report the 2.5 Å resolution crystal structure of the complete C-terminal region of AgI/II. The C-terminal region is comprised of three major domains: C(1), C(2), and C(3). Each domain adopts a DE-variant IgG fold, with two β-sheets whose A and F strands are linked through an intramolecular isopeptide bond. The adherence of the C-terminal AgI/II fragments to the putative tooth surface receptor salivary agglutinin (SAG), as monitored by surface plasmon resonance, indicated that the minimal region of binding was contained within the first and second DE-variant-IgG domains (C(1) and C(2)) of the C terminus. The minimal C-terminal region that could inhibit S. mutans adherence to SAG was also confirmed to be within the C(1) and C(2) domains. Competition experiments demonstrated that the C- and N-terminal regions of AgI/II adhere to distinct sites on SAG. A cleft formed at the intersection between these C(1) and C(2) domains bound glucose molecules from the cryo-protectant solution, revealing a putative binding site for its highly glycosylated receptor SAG. Finally, electron microscopy images confirmed the elongated structure of AgI/II and enabled building a composite tertiary model that encompasses its two distinct binding regions.

摘要

变异链球菌抗原 I/II(AgI/II)是一种位于细胞表面的蛋白质,可黏附于唾液成分和细胞外基质分子。在此,我们报告了 AgI/II 完整 C 端区域的 2.5 Å 分辨率晶体结构。C 端区域由三个主要结构域组成:C(1)、C(2)和 C(3)。每个结构域均采用 DE 变体 IgG 折叠,由两条β-折叠组成,其 A 和 F 链通过分子内异肽键连接。通过表面等离子体共振监测,C 端 AgI/II 片段与假定的牙齿表面受体唾液黏附素(SAG)的黏附表明,结合的最小区域包含在 C 端的第一个和第二个 DE 变体-IgG 结构域(C(1)和 C(2))内。能够抑制 S. mutans 与 SAG 黏附的最小 C 端区域也被证实位于 C(1)和 C(2)结构域内。竞争实验表明,AgI/II 的 C 端和 N 端区域与 SAG 上的不同位点结合。在这些 C(1)和 C(2)结构域的交汇处形成的裂缝结合了来自低温保护剂溶液中的葡萄糖分子,揭示了其高度糖基化受体 SAG 的潜在结合位点。最后,电子显微镜图像证实了 AgI/II 的长形结构,并能够构建包含其两个不同结合区域的复合三级模型。

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