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具有新型 Ig 样折叠的细菌蛋白结构域靶向人 CEACAM 受体。

Bacterial protein domains with a novel Ig-like fold target human CEACAM receptors.

机构信息

Department of Medical Microbiology, University Medical Center Utrecht, Utrecht University, Utrecht, The Netherlands.

Institute of Human Virology, University of Maryland School of Medicine, University of Maryland, Baltimore, MD, USA.

出版信息

EMBO J. 2021 Apr 1;40(7):e106103. doi: 10.15252/embj.2020106103. Epub 2021 Feb 1.

Abstract

Streptococcus agalactiae, also known as group B Streptococcus (GBS), is the major cause of neonatal sepsis in humans. A critical step to infection is adhesion of bacteria to epithelial surfaces. GBS adhesins have been identified to bind extracellular matrix components and cellular receptors. However, several putative adhesins have no host binding partner characterised. We report here that surface-expressed β protein of GBS binds to human CEACAM1 and CEACAM5 receptors. A crystal structure of the complex showed that an IgSF domain in β represents a novel Ig-fold subtype called IgI3, in which unique features allow binding to CEACAM1. Bioinformatic assessment revealed that this newly identified IgI3 fold is not exclusively present in GBS but is predicted to be present in adhesins from other clinically important human pathogens. In agreement with this prediction, we found that CEACAM1 binds to an IgI3 domain found in an adhesin from a different streptococcal species. Overall, our results indicate that the IgI3 fold could provide a broadly applied mechanism for bacteria to target CEACAMs.

摘要

无乳链球菌,亦称 B 群链球菌(GBS),是导致人类新生儿败血症的主要原因。感染的关键步骤是细菌黏附到上皮表面。现已鉴定出 GBS 黏附素可结合细胞外基质成分和细胞受体。然而,一些假定的黏附素尚无特征明确的宿主结合配体。我们在此报告 GBS 表面表达的 β 蛋白可与人类 CEACAM1 和 CEACAM5 受体结合。复合物的晶体结构显示,β 中的一个 IgSF 结构域代表了一种新型的 Ig 折叠亚型,称为 IgI3,其独特的特征允许与 CEACAM1 结合。生物信息学评估显示,这种新鉴定的 IgI3 折叠不仅存在于 GBS 中,而且预计存在于其他临床上重要的人类病原体的黏附素中。与这一预测一致,我们发现 CEACAM1 与另一种链球菌种黏附素中的 IgI3 结构域结合。总体而言,我们的结果表明,IgI3 折叠可能为细菌靶向 CEACAMs 提供了一种广泛应用的机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f1e/8013792/ea9e8f6512c3/EMBJ-40-e106103-g012.jpg

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