Human Vaccines & Immunotherapeutics (Jun 2018)

Levels of regulatory B cells do not predict serological responses to hepatitis B vaccine

  • Maria Bolther,
  • Karen Lise Dahl Andersen,
  • Martin Tolstrup,
  • Kumar Visvanathan,
  • Ian Woolley,
  • Narelle Skinner,
  • Rosemary Millen,
  • Nadia Warner,
  • Lars Østergaard,
  • Søren Jensen-Fangel

DOI
https://doi.org/10.1080/21645515.2018.1441653
Journal volume & issue
Vol. 14, no. 6
pp. 1483 – 1488

Abstract

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This study investigated the immunomodulatory influence of IL10 producing B regulatory cells, Bregs (CD19+CD24hiCD38hi) to standard Twinrix® vaccination. We also investigated HBsAg specific T-cell mediated IFN-γ responses to Twinrix® which in theory could provide effective immunity despite low anti-HBs titer. A total of 309 hepatitis B negative health care students and workers completed a standard Twinrix® vaccination schedule (0, 1 and 6 months). Depending on the vaccination response the participants were divided in to non-, low- and high responders according to anti-HBs titer (1000 mIU/mL respectively) two months after completed vaccination schedule. Blood samples from baseline and after vaccination from all non- and low-responders (23 participants) and the same number of high-responders were used for flow cytometric analyses of IL10 producing Bregs and T-cell mediated IFN-γ responses. A decrease in levels of IL10 producing Bregs was observed after vaccination in high responders compared to non- and low-responders. Compiling non-and low-responders against high-responders showed a lower T-cell mediated IFN-γ response at baseline in non-and low-responders when stimulated with Engerix® vaccine. In contrary no positive correlation between IL10 producing Bregs or IFN-γ positive T-cells and anti-HBs titer was observed. Hence this study cannot prove that levels of IL10 producing Bregs or IFN-γ positive T cell affect HBV vaccine response.

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