Pangenome analysis and virulence profiling of Streptococcus intermedius
Abstract Background Streptococcus intermedius, a member of the S. anginosus group, is a commensal bacterium present in the normal microbiota of human mucosal surfaces of the oral, gastrointestinal, and urogenital tracts. However, it has been associated with various infections such as liver and brain...
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doaj-8488f6ab34fd4214898009c9bb6b99052021-07-11T11:32:28ZengBMCBMC Genomics1471-21642021-07-0122111710.1186/s12864-021-07829-2Pangenome analysis and virulence profiling of Streptococcus intermediusDhiraj Sinha0Xifeng Sun1Mudra Khare2Michel Drancourt3Didier Raoult4Pierre-Edouard Fournier5Aix-Marseille University, IRD, AP-HM, SSA, VITROME, IHU Méditerranée InfectionAix-Marseille University, IRD, AP-HM, SSA, VITROME, IHU Méditerranée InfectionAix-Marseille University, IRD, AP-HM, SSA, VITROME, IHU Méditerranée InfectionIHU Méditerranée InfectionIHU Méditerranée InfectionAix-Marseille University, IRD, AP-HM, SSA, VITROME, IHU Méditerranée InfectionAbstract Background Streptococcus intermedius, a member of the S. anginosus group, is a commensal bacterium present in the normal microbiota of human mucosal surfaces of the oral, gastrointestinal, and urogenital tracts. However, it has been associated with various infections such as liver and brain abscesses, bacteremia, osteo-articular infections, and endocarditis. Since 2005, high throughput genome sequencing methods enabled understanding the genetic landscape and diversity of bacteria as well as their pathogenic role. Here, in order to determine whether specific virulence genes could be related to specific clinical manifestations, we compared the genomes from 27 S. intermedius strains isolated from patients with various types of infections, including 13 that were sequenced in our institute and 14 available in GenBank. Results We estimated the theoretical pangenome size to be of 4,020 genes, including 1,355 core genes, 1,054 strain-specific genes and 1,611 accessory genes shared by 2 or more strains. The pangenome analysis demonstrated that the genomic diversity of S. intermedius represents an “open” pangenome model. We identified a core virulome of 70 genes and 78 unique virulence markers. The phylogenetic clusters based upon core-genome sequences and SNPs were independent from disease types and sample sources. However, using Principal Component analysis based on presence/ absence of virulence genes, we identified the sda histidine kinase, adhesion protein LAP and capsular polysaccharide biosynthesis protein cps4E as being associated to brain abscess or broncho-pulmonary infection. In contrast, liver and abdominal abscess were associated to presence of the fibronectin binding protein fbp54 and capsular polysaccharide biosynthesis protein cap8D and cpsB. Conclusions Based on the virulence gene content of 27 S. intermedius strains causing various diseases, we identified putative disease-specific genetic profiles discriminating those causing brain abscess or broncho-pulmonary infection from those causing liver and abdominal abscess. These results provide an insight into S. intermedius pathogenesis and highlights putative targets in a diagnostic perspective.https://doi.org/10.1186/s12864-021-07829-2Streptococcus intermediusStreptococcus anginosus groupInfectionVirulenceComparative genomicsWhole genome sequencing |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Dhiraj Sinha Xifeng Sun Mudra Khare Michel Drancourt Didier Raoult Pierre-Edouard Fournier |
spellingShingle |
Dhiraj Sinha Xifeng Sun Mudra Khare Michel Drancourt Didier Raoult Pierre-Edouard Fournier Pangenome analysis and virulence profiling of Streptococcus intermedius BMC Genomics Streptococcus intermedius Streptococcus anginosus group Infection Virulence Comparative genomics Whole genome sequencing |
author_facet |
Dhiraj Sinha Xifeng Sun Mudra Khare Michel Drancourt Didier Raoult Pierre-Edouard Fournier |
author_sort |
Dhiraj Sinha |
title |
Pangenome analysis and virulence profiling of Streptococcus intermedius |
title_short |
Pangenome analysis and virulence profiling of Streptococcus intermedius |
title_full |
Pangenome analysis and virulence profiling of Streptococcus intermedius |
title_fullStr |
Pangenome analysis and virulence profiling of Streptococcus intermedius |
title_full_unstemmed |
Pangenome analysis and virulence profiling of Streptococcus intermedius |
title_sort |
pangenome analysis and virulence profiling of streptococcus intermedius |
publisher |
BMC |
series |
BMC Genomics |
issn |
1471-2164 |
publishDate |
2021-07-01 |
description |
Abstract Background Streptococcus intermedius, a member of the S. anginosus group, is a commensal bacterium present in the normal microbiota of human mucosal surfaces of the oral, gastrointestinal, and urogenital tracts. However, it has been associated with various infections such as liver and brain abscesses, bacteremia, osteo-articular infections, and endocarditis. Since 2005, high throughput genome sequencing methods enabled understanding the genetic landscape and diversity of bacteria as well as their pathogenic role. Here, in order to determine whether specific virulence genes could be related to specific clinical manifestations, we compared the genomes from 27 S. intermedius strains isolated from patients with various types of infections, including 13 that were sequenced in our institute and 14 available in GenBank. Results We estimated the theoretical pangenome size to be of 4,020 genes, including 1,355 core genes, 1,054 strain-specific genes and 1,611 accessory genes shared by 2 or more strains. The pangenome analysis demonstrated that the genomic diversity of S. intermedius represents an “open” pangenome model. We identified a core virulome of 70 genes and 78 unique virulence markers. The phylogenetic clusters based upon core-genome sequences and SNPs were independent from disease types and sample sources. However, using Principal Component analysis based on presence/ absence of virulence genes, we identified the sda histidine kinase, adhesion protein LAP and capsular polysaccharide biosynthesis protein cps4E as being associated to brain abscess or broncho-pulmonary infection. In contrast, liver and abdominal abscess were associated to presence of the fibronectin binding protein fbp54 and capsular polysaccharide biosynthesis protein cap8D and cpsB. Conclusions Based on the virulence gene content of 27 S. intermedius strains causing various diseases, we identified putative disease-specific genetic profiles discriminating those causing brain abscess or broncho-pulmonary infection from those causing liver and abdominal abscess. These results provide an insight into S. intermedius pathogenesis and highlights putative targets in a diagnostic perspective. |
topic |
Streptococcus intermedius Streptococcus anginosus group Infection Virulence Comparative genomics Whole genome sequencing |
url |
https://doi.org/10.1186/s12864-021-07829-2 |
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