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Review
. 2021 Oct;131(4):1600-1620.
doi: 10.1111/jam.15090. Epub 2021 Apr 7.

A current review of pathogenicity determinants of Streptococcus sp

P S Lannes-Costa  1 J S S de Oliveira  1 G da Silva Santos  1 P E Nagao  1
Affiliations
Review

A current review of pathogenicity determinants of Streptococcus sp

P S Lannes-Costa et al. J Appl Microbiol. 2021 Oct.

Abstract

The genus Streptococcus comprises important pathogens, many of them are part of the human or animal microbiota. Advances in molecular genetics, taxonomic approaches and phylogenomic studies have led to the establishment of at least 100 species that have a severe impact on human health and are responsible for substantial economic losses to agriculture. The infectivity of the pathogens is linked to cell-surface components and/or secreted virulence factors. Bacteria have evolved sophisticated and multifaceted adaptation strategies to the host environment, including biofilm formation, survival within professional phagocytes, escape the host immune response, amongst others. This review focuses on virulence mechanism and zoonotic potential of Streptococcus species from pyogenic (S. agalactiae, S. pyogenes) and mitis groups (S. pneumoniae).

Keywords: diseases; infection; pathogenesis; streptococci; virulence.

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References

    1. Agarwal, V., Sroka, M., Fulde, M., Bergmann, S., Riesbeck, K. and Blom, A.M. (2014) Binding of Streptococcus pneumoniae endopeptidase O (PepO) to complement component C1q modulates the complement attack and promotes host cell adherence. J Biol Chem 289, 15833-15844.
    1. Al Safadi, R., Mereghetti, L., Salloum, M., Lartigue, M.F., Virlogeux-Payant, I., Quentin, R. and Rosenau, A. (2011) Two-component system RgfA/C activates the fbsB gene encoding major fibrinogen-binding protein in highly virulent CC17 clone group B Streptococcus. PLoS One 6, e14658.
    1. Andrade, W., Firon, A., Schmidt, T., Hornung, V., Fitzgerald, K., Kurt-Jones, E., Trieu-Cuot, P., Golenbock, D. et al. (2016) Group B Streptococcus degrades cyclic-di-AMP to modulate STING-dependent type I interferon production. Cell Host Microbe 20, 49-59.
    1. Andre, G.O., Converso, T.R., Politano, W.R., Ferraz, L.F., Ribeiro, M.L., Leite, L.C. and Darrieux, M. (2017) Role of Streptococcus pneumoniae proteins in evasion of complement-mediated immunity. Front Microbiol 8, 224.
    1. Armistead, B., Oler, E., Adams, W.K. and Rajagopal, L. (2019) The double life of group B streptococcus: asymptomatic colonizer and potent pathogen. J Mol Biol 431, 2914-2931.

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