Cristin-resultat-ID: 1597995
Sist endret: 8. februar 2019, 17:31
NVI-rapporteringsår: 2018
Resultat
Vitenskapelig artikkel
2018

Antibodies reactive to commensal Streptococcus mitis show cross-reactivity with virulent Streptococcus pneumoniae serotypes

Bidragsytere:
  • Sudhanshu Shekhar
  • Rabia Khan
  • Daniela M. Ferreira
  • Elena Mitsi
  • Esther German
  • Gro Herredsvela Rørvik
  • mfl.

Tidsskrift

Frontiers in Immunology
ISSN 1664-3224
e-ISSN 1664-3224
NVI-nivå 1

Om resultatet

Vitenskapelig artikkel
Publiseringsår: 2018
Volum: 9:747
Sider: 1 - 10
Open Access

Importkilder

Scopus-ID: 2-s2.0-85045471327

Klassifisering

Vitenskapsdisipliner

Basale medisinske, odontologiske og veterinærmedisinske fag

Emneord

Immunologi

Beskrivelse Beskrivelse

Tittel

Antibodies reactive to commensal Streptococcus mitis show cross-reactivity with virulent Streptococcus pneumoniae serotypes

Sammendrag

Current vaccines against Streptococcus pneumoniae, a bacterial species that afflicts people by causing a wide spectrum of diseases, do not protect against all pneumococcal serotypes. Thus, alternative vaccines to fight pneumococcal infections that target common proteins are under investigation. One promising strategy is to take advantage of immune cross-reactivity between commensal and pathogenic microbes for cross-protection. In this study, we examined the antibody-mediated cross-reactivity between S. pneumoniae and Streptococcus mitis, a commensal species closely related to S. pneumoniae. Western blot analysis showed that rabbit antisera raised against S. mitis reacted with multiple proteins of virulent S. pneumoniae strains (6B, TIGR4, and D39). Rabbit anti-S. pneumoniae IgG antibodies also showed binding to S. mitis antigens. Incubation of rabbit antisera raised against S. mitis with heterologous or homologous bacterial lysates resulted in marked inhibition of the developments of bands in the Western blots. Furthermore, plasma IgG antibodies from adult human volunteers intranasally inoculated with S. pneumoniae 6B revealed enhanced S. mitis-specific IgG titers compared with the pre-inoculation samples. Using an on-chip protein microarray representing a number of selected membrane and extracellular S. pneumoniae proteins, we identified choline-binding protein D (CbpD), cell division protein (FtsH), and manganese ABC transporter or manganese-binding adhesion lipoprotein (PsaA) as common targets of the rabbit IgG antibodies raised against S. mitis or S. pneumoniae. Cumulatively, these findings provide evidence on the antibody-mediated cross-reactivity of proteins from S. mitis and S. pneumoniae, which may have implications for development of effective and wide-range pneumococcal vaccines.

Bidragsytere

Sudhanshu Shekhar

  • Tilknyttet:
    Forfatter
    ved Institutt for oral biologi ved Universitetet i Oslo

Rabia Khan

  • Tilknyttet:
    Forfatter
    ved Institutt for oral biologi ved Universitetet i Oslo

Daniela M. Ferreira

  • Tilknyttet:
    Forfatter
    ved Liverpool School of Tropical Medicine

Elena Mitsi

  • Tilknyttet:
    Forfatter
    ved Liverpool School of Tropical Medicine

Esther German

  • Tilknyttet:
    Forfatter
    ved Liverpool School of Tropical Medicine
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