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Genomic and panproteomic analysis of the development of infant immune responses to antigenically-diverse pneumococci

Author

Listed:
  • Nicholas J. Croucher

    (School of Public Health, Imperial College London)

  • Joseph J. Campo

    (Antigen Discovery Inc)

  • Timothy Q. Le

    (Antigen Discovery Inc)

  • Jozelyn V. Pablo

    (Antigen Discovery Inc)

  • Christopher Hung

    (Antigen Discovery Inc)

  • Andy A. Teng

    (Antigen Discovery Inc)

  • Claudia Turner

    (Cambodia Oxford Medical Research Unit, Angkor Hospital for Children
    University of Oxford)

  • François Nosten

    (University of Oxford
    Mahidol University)

  • Stephen D. Bentley

    (Wellcome Sanger Institute, Wellcome Genome Campus)

  • Xiaowu Liang

    (Antigen Discovery Inc)

  • Paul Turner

    (Cambodia Oxford Medical Research Unit, Angkor Hospital for Children
    University of Oxford)

  • David Goldblatt

    (University College London)

Abstract

Streptococcus pneumoniae (pneumococcus) is a nasopharyngeal commensal and respiratory pathogen. This study characterises the immunoglobulin G (IgG) repertoire recognising pneumococci from birth to 24 months old (mo) in a prospectively-sampled cohort of 63 children using a panproteome array. IgG levels are highest at birth, due to transplacental transmission of maternal antibodies. The subsequent emergence of responses to individual antigens exhibit distinct kinetics across the cohort. Stable differences in the strength of individuals’ responses, correlating with maternal IgG concentrations, are established by 6 mo. By 12 mo, children develop unique antibody profiles that are boosted by re-exposure. However, some proteins only stimulate substantial responses in adults. Integrating genomic data on nasopharyngeal colonisation demonstrates rare pneumococcal antigens can elicit strong IgG levels post-exposure. Quantifying such responses to the diverse core loci (DCL) proteins is complicated by cross-immunity between variants. In particular, the conserved N terminus of DCL protein zinc metalloprotease B provokes the strongest early IgG responses. DCL proteins’ ability to inhibit mucosal immunity likely explains continued pneumococcal carriage despite hosts’ polyvalent antibody repertoire. Yet higher IgG levels are associated with reduced incidence, and severity, of pneumonia, demonstrating the importance of the heterogeneity in response strength and kinetics across antigens and individuals.

Suggested Citation

  • Nicholas J. Croucher & Joseph J. Campo & Timothy Q. Le & Jozelyn V. Pablo & Christopher Hung & Andy A. Teng & Claudia Turner & François Nosten & Stephen D. Bentley & Xiaowu Liang & Paul Turner & David, 2024. "Genomic and panproteomic analysis of the development of infant immune responses to antigenically-diverse pneumococci," Nature Communications, Nature, vol. 15(1), pages 1-20, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-023-44584-2
    DOI: 10.1038/s41467-023-44584-2
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    References listed on IDEAS

    as
    1. Zhiming Wang & Jeremy Rahkola & Jasmina S. Redzic & Ying-Chih Chi & Norman Tran & Todd Holyoak & Hongjin Zheng & Edward Janoff & Elan Eisenmesser, 2020. "Mechanism and inhibition of Streptococcus pneumoniae IgA1 protease," Nature Communications, Nature, vol. 11(1), pages 1-8, December.
    2. Alessandra Løchen & James E Truscott & Nicholas J Croucher, 2022. "Analysing pneumococcal invasiveness using Bayesian models of pathogen progression rates," PLOS Computational Biology, Public Library of Science, vol. 18(2), pages 1-37, February.
    3. Bates, Douglas & Mächler, Martin & Bolker, Ben & Walker, Steve, 2015. "Fitting Linear Mixed-Effects Models Using lme4," Journal of Statistical Software, Foundation for Open Access Statistics, vol. 67(i01).
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