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糖蛋白340富含清道夫的半胱氨酸重复序列(SRCR)结构域的钙诱导构象和糖基化影响其与抗原I/II同源物的高亲和力相互作用。

The calcium-induced conformation and glycosylation of scavenger-rich cysteine repeat (SRCR) domains of glycoprotein 340 influence the high affinity interaction with antigen I/II homologs.

作者信息

Purushotham Sangeetha, Deivanayagam Champion

机构信息

From the Department of Vision Sciences/Center for Structural Biology, University of Alabama at Birmingham, Birmingham, Alabama 35294-4400.

From the Department of Vision Sciences/Center for Structural Biology, University of Alabama at Birmingham, Birmingham, Alabama 35294-4400

出版信息

J Biol Chem. 2014 Aug 8;289(32):21877-87. doi: 10.1074/jbc.M114.565507. Epub 2014 Jun 12.

Abstract

Oral streptococci adhere to tooth-immobilized glycoprotein 340 (GP340) via the surface protein antigen I/II (AgI/II) and its homologs as the first step in pathogenesis. Studying this interaction using recombinant proteins, we observed that calcium increases the conformational stability of the scavenger-rich cysteine repeat (SRCRs) domains of GP340. Our results also show that AgI/II adheres specifically with nanomolar affinity to the calcium-induced SRCR conformation in an immobilized state and not in solution. This interaction is significantly dependent on the O-linked carbohydrates present on the SRCRs. This study also establishes that a single SRCR domain of GP340 contains the two surfaces to which the apical and C-terminal regions of AgI/II noncompetitively adhere. Compared with the single SRCR domain, the three tandem SRCR domains displayed a collective/cooperative increase in their bacterial adherence and aggregation. The previously described SRCRP2 peptide that was shown to aggregate several oral streptococci displayed limited aggregation and also nonspecific adherence compared to SRCR domains. Finally, we show distinct species-specific adherence/aggregation between Streptococcus mutans AgI/II and Streptococcus gordonii SspB in their interaction with the SRCRs. This study concludes that identification of the metal ion and carbohydrate adherence motifs on both SRCRs and AgI/II homologs could lead to the development of anti-adhesive inhibitors that could deter the adherence of pathogenic oral streptococci and thereby prevent the onset of infections.

摘要

口腔链球菌通过表面蛋白抗原I/II(AgI/II)及其同源物粘附于固定在牙齿上的糖蛋白340(GP340),这是发病机制的第一步。使用重组蛋白研究这种相互作用时,我们观察到钙可增加GP340富含清道夫的半胱氨酸重复序列(SRCRs)结构域的构象稳定性。我们的结果还表明,AgI/II以纳摩尔亲和力特异性粘附于固定状态而非溶液状态下钙诱导的SRCR构象。这种相互作用显著依赖于SRCRs上存在的O-连接碳水化合物。本研究还确定,GP340的单个SRCR结构域包含AgI/II顶端和C末端区域非竞争性粘附的两个表面。与单个SRCR结构域相比,三个串联的SRCR结构域在细菌粘附和聚集方面表现出集体/协同增加。与SRCR结构域相比,先前描述的可聚集几种口腔链球菌的SRCRP2肽表现出有限的聚集以及非特异性粘附。最后,我们展示了变形链球菌AgI/II和戈登链球菌SspB在与SRCRs相互作用时明显的物种特异性粘附/聚集。本研究得出结论,鉴定SRCRs和AgI/II同源物上的金属离子和碳水化合物粘附基序可能会导致开发出抗粘附抑制剂,从而阻止致病性口腔链球菌的粘附,进而预防感染的发生。

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本文引用的文献

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Protein Expr Purif. 2013 Aug;90(2):67-73. doi: 10.1016/j.pep.2013.05.003. Epub 2013 May 22.
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Innate Immun. 2010 Jun;16(3):160-7. doi: 10.1177/1753425910368447. Epub 2010 Apr 23.

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