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葡萄球菌超抗原样蛋白 4 的结构和功能特性。

Structural and functional properties of staphylococcal superantigen-like protein 4.

机构信息

School of Medical Sciences, University of Auckland, Aukland, New Zealand.

出版信息

Infect Immun. 2012 Nov;80(11):4004-13. doi: 10.1128/IAI.00764-12. Epub 2012 Sep 4.

Abstract

Staphylococcus aureus is a prevalent and significant human pathogen. Among the repertoire of virulence factors produced by this bacterium are the 14 staphylococcal superantigen-like (SSL) proteins. SSL protein 4 (SSL4) is one member of this family and contains a highly conserved carbohydrate binding site also found in SSL2, SSL3, SSL5, SSL6, and SSL11. Recombinant SSL4(t), comprising amino acids 109 to 309 of Newman strain SSL4 (SSL4-Newman), has been shown to bind and be internalized by human granulocytes and macrophages in a sialic-acid (Sia)-dependent manner. SSL4(t) can compete with itself for cell binding, indicating that binding is target specific. A 2.5-Å-resolution crystal structure of SSL4(t) complexed with sialyl Lewis X (sLe(x)) [sLe(x)-Neu5Acα2-3Galβ1-4(Fucα1-3)GlcNAc] revealed a similar binding site to SSL5 and SSL11. These data, along with data on SSL4(t) binding to a glycan array and biosensor analysis of sLe(x) and sialyllactosamine (sLacNac) binding are compared with those for SSL11. Although these proteins show great similarity in their carbohydrate binding sites, with a root mean square (RMS) difference between main chain atom positions of only 0.34 Å, these proteins differ in detail in their affinity for sLe(x) and sLacNac, as well as their glycan preference. Together with cell binding data, this shows how S. aureus produces multiple related proteins that target myeloid cells through specific sialyllactosamine-containing glycoproteins.

摘要

金黄色葡萄球菌是一种普遍且重要的人类病原体。这种细菌产生的多种毒力因子中,包括 14 种葡萄球菌超抗原样(SSL)蛋白。SSL 蛋白 4(SSL4)是该家族的一个成员,其含有一个高度保守的碳水化合物结合位点,也存在于 SSL2、SSL3、SSL5、SSL6 和 SSL11 中。含有纽马克菌株 SSL4(SSL4-Newman)109 至 309 个氨基酸的重组 SSL4(t) 已被证明以唾液酸(Sia)依赖性方式结合并被人类粒细胞和巨噬细胞内化。SSL4(t) 可以与自身竞争细胞结合,表明结合具有特异性。SSL4(t) 与唾液酸化路易斯 X(sLe(x))[sLe(x)-Neu5Acα2-3Galβ1-4(Fucα1-3)GlcNAc] 复合物的 2.5-Å 分辨率晶体结构揭示了与 SSL5 和 SSL11 相似的结合位点。这些数据,以及 SSL4(t) 与聚糖阵列的结合数据和 sLe(x) 和唾液酸乳糖胺(sLacNac)结合的生物传感器分析,与 SSL11 的进行了比较。尽管这些蛋白在其碳水化合物结合位点上具有很大的相似性,主链原子位置的均方根(RMS)差异仅为 0.34 Å,但它们在 sLe(x) 和 sLacNac 的亲和力以及糖基偏好方面存在差异。结合细胞结合数据,这表明金黄色葡萄球菌如何通过特定的含有唾液酸乳糖胺的糖蛋白产生多种靶向髓样细胞的相关蛋白。

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