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Sara Larsson

Research engineer

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A group B Streptococcus alpha-like protein subunit vaccine induces functionally active antibodies in humans targeting homotypic and heterotypic strains

Author

  • Andrzej Pawlowski
  • Jonas Lannergård
  • Majela Gonzalez-Miro
  • Duojia Cao
  • Sara Larsson
  • Jenny J. Persson
  • Geoff Kitson
  • Michael Darsley
  • Ane Lilleøre Rom
  • Morten Hedegaard
  • Per B. Fischer
  • Bengt Johansson-Lindbom

Summary, in English

Maternal vaccination is a promising strategy for preventing neonatal disease caused by group B Streptococcus. The safety and immunogenicity of the prototype vaccine GBS-NN, a fusion protein consisting of the N-terminal domains of the alpha-like proteins (Alp) αC and Rib, were recently evaluated favorably in healthy adult women in a phase 1 trial. Here we demonstrate robust immunoglobulin G (IgG) and immunoglobulin A (IgA) responses against αC and Rib, as well as against the heterotypic Alp family members Alp1–Alp3. IgA and heterotypic IgG responses are more variable between subjects and correlate with pre-existing immunity. Vaccine-induced IgG mediates opsonophagocytic killing and prevents bacterial invasion of epithelial cells. Like the vaccine-induced response, naturally acquired IgG against the vaccine domains is dominated by IgG1. Consistent with the high IgG1 cross-placental transfer rate, naturally acquired IgG against both domains reaches higher concentrations in neonatal than maternal blood, as assessed in a separate group of non-vaccinated pregnant women and their babies.

Department/s

  • Adaptive Immunity
  • Host-Pathogen Interactions

Publishing year

2022

Language

English

Publication/Series

Cell Reports Medicine

Volume

3

Issue

2

Document type

Journal article

Publisher

Elsevier

Topic

  • Microbiology in the medical area
  • Infectious Medicine

Keywords

  • antibodies
  • group B Streptococcus
  • maternal immunization
  • neonatal disease
  • opsonophagocytosis
  • vaccines

Status

Published

Research group

  • Adaptive Immunity
  • Host-Pathogen Interactions

ISBN/ISSN/Other

  • ISSN: 2666-3791