| Literature DB >> 26094503 |
Anne Six1,2,3,4, Samuel Bellais1,2,3,4, Abdelouhab Bouaboud1,2,3,4, Agnès Fouet1,2,3,4,5, Christelle Gabriel1,2,3,4, Asmaa Tazi1,2,3,4,5,6, Shaynoor Dramsi7,8, Patrick Trieu-Cuot7,8, Claire Poyart1,2,3,4,7,8,5,6.
Abstract
The Group B Streptococcus (GBS) 'hypervirulent' ST-17 clone is strongly associated with invasive neonatal meningitis. Comparative genome analyses revealed that the serine-rich repeat (Srr) glycoprotein Srr2 is a cell wall-anchored protein specific for ST-17 strains, the non-ST-17 isolates expressing Srr1. Here, we unravel the binding capacity of GBS Srr proteins to relevant components of the host fibrinolysis pathway. We demonstrate that: (i) Srr2 binds plasminogen and plasmin whereas Srr1 does not; (ii) the ability of ST-17 strains to bind fibrinogen reflects a high level surface display of Srr2 combined with a higher affinity of Srr2 than Srr1 to bind this ligand; and (iii) Srr2 binding to host plasma proteins results in the formation of bacterial aggregates that are efficiently endocytosed by phagocytes. Importantly, we show that Srr2 increased bacterial survival to phagocytic killing and bacterial persistence in a murine model of meningitis. We conclude that Srr2 is a multifaceted adhesin used by the ST-17 clone to hijack ligands of the host coagulation system, thereby contributing to bacterial dissemination and invasiveness, and ultimately to meningitis.Entities:
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Year: 2015 PMID: 26094503 DOI: 10.1111/mmi.13097
Source DB: PubMed Journal: Mol Microbiol ISSN: 0950-382X Impact factor: 3.501