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Analysis of B Cell Repertoire Dynamics Following Hepatitis B Vaccination in Humans, and Enrichment of Vaccine-specific Antibody Sequences
Author(s) -
Jacob D. Galson,
Johannes Trück,
Anna Fowler,
Elizabeth Clutterbuck,
Márton Münz,
Vincenzo Cerundolo,
Claudia Reinhard,
Robbert van der Most,
Andrew J. Pollard,
Gerton Lunter,
Dominic F. Kelly
Publication year - 2015
Publication title -
ebiomedicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.596
H-Index - 63
ISSN - 2352-3964
DOI - 10.1016/j.ebiom.2015.11.034
Subject(s) - repertoire , antibody repertoire , biology , vaccination , complementarity determining region , virology , antibody , immunology , antigen , immunogenicity , computational biology , genetics , monoclonal antibody , physics , acoustics
Generating a diverse B cell immunoglobulin repertoire is essential for protection against infection. The repertoire in humans can now be comprehensively measured by high-throughput sequencing. Using hepatitis B vaccination as a model, we determined how the total immunoglobulin sequence repertoire changes following antigen exposure in humans, and compared this to sequences from vaccine-specific sorted cells. Clonal sequence expansions were seen 7 days after vaccination, which correlated with vaccine-specific plasma cell numbers. These expansions caused an increase in mutation, and a decrease in diversity and complementarity-determining region 3 sequence length in the repertoire. We also saw an increase in sequence convergence between participants 14 and 21 days after vaccination, coinciding with an increase of vaccine-specific memory cells. These features allowed development of a model for in silico enrichment of vaccine-specific sequences from the total repertoire. Identifying antigen-specific sequences from total repertoire data could aid our understanding B cell driven immunity, and be used for disease diagnostics and vaccine evaluation.

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