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链球菌类 Siglec 黏附素识别不同的人血浆糖蛋白亚群:对感染性心内膜炎的影响。

Streptococcal Siglec-like adhesins recognize different subsets of human plasma glycoproteins: implications for infective endocarditis.

机构信息

Department of Medicine, San Francisco Veterans Affairs Medical Center and University of California, San Francisco, CA, USA.

Department of Chemistry, University of California, Davis, CA, USA.

出版信息

Glycobiology. 2018 Aug 1;28(8):601-611. doi: 10.1093/glycob/cwy052.

Abstract

Streptococcus gordonii and Streptococcus sanguinis are typically found among the normal oral microbiota but can also cause infective endocarditis. These organisms express cell surface serine-rich repeat adhesins containing "Siglec-like" binding regions (SLBRs) that mediate attachment to α2-3-linked sialic acids on human glycoproteins. Two known receptors for the Siglec-like adhesins are the salivary mucin MG2/MUC7 and platelet GPIbα, and the interaction of streptococci with these targets may contribute to oral colonization and endocarditis, respectively. The SLBRs display a surprising diversity of preferences for defined glycans, ranging from highly selective to broader specificity. In this report, we characterize the glycoproteins in human plasma recognized by four SLBRs that prefer different α2-3 sialoglycan structures. We found that the SLBRs recognize a surprisingly small subset of plasma proteins that are extensively O-glycosylated. The preferred plasma protein ligands for a sialyl-T antigen-selective SLBR are proteoglycan 4 (lubricin) and inter-alpha-trypsin inhibitor heavy chain H4. Conversely, the preferred ligand for a 3'sialyllactosamine-selective SLBR is glycocalicin (the extracellular portion of platelet GPIbα). All four SLBRs recognize C1 inhibitor but detect distinctly different glycoforms of this key regulator of the complement and kallikrein protease cascades. The four plasma ligands have potential roles in thrombosis and inflammation, and each has been cited as a biomarker for one or more vascular or other diseases. The combined results suggest that the interaction of Siglec-like adhesins with different subsets of plasma glycoproteins could have a significant impact on the propensity of streptococci to establish endocardial infections.

摘要

戈登链球菌和中间链球菌通常存在于正常的口腔微生物群中,但也可引起感染性心内膜炎。这些生物体表达细胞表面富含丝氨酸的重复黏附素,其中含有介导与人类糖蛋白上的α2-3 连接唾液酸结合的“Siglec 样”结合区(SLBR)。Siglec 样黏附素的两个已知受体是唾液黏蛋白 MG2/MUC7 和血小板 GPIbα,链球菌与这些靶标的相互作用分别有助于口腔定植和心内膜炎。SLBR 对特定糖链表现出惊人的多样性偏好,从高度选择性到更广泛的特异性。在本报告中,我们描述了四个偏好不同α2-3 唾液酸化糖结构的 SLBR 识别的人血浆糖蛋白。我们发现,SLBR 识别出人血浆蛋白中一个非常小的子集,这些蛋白广泛地发生 O-糖基化。对唾液酰-T 抗原选择性 SLBR 具有偏好性的血浆蛋白配体是蛋白聚糖 4(润滑素)和抗胰蛋白酶抑制剂重链 H4。相反,对 3'唾液酸乳糖胺选择性 SLBR 的首选配体是糖钙蛋白(血小板 GPIbα 的细胞外部分)。所有四个 SLBR 都识别 C1 抑制剂,但检测到这种补体和激肽蛋白酶级联关键调节剂的不同糖型。这四个血浆配体在血栓形成和炎症中具有潜在作用,并且每个配体都被认为是一种或多种血管或其他疾病的生物标志物。综合结果表明,Siglec 样黏附素与不同亚群的血浆糖蛋白的相互作用可能对链球菌建立心内膜感染的倾向产生重大影响。

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