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A transgenic mouse with a humanised B cell repertoire mounts an antibody response to influenza infection and vaccination

Murugaiah, V., Watson, S.J., Cunliffe, R.F., Temperton, Nigel J., Reece, S.T., Kellam, P., Tregoning, J.S. (2024) A transgenic mouse with a humanised B cell repertoire mounts an antibody response to influenza infection and vaccination. The Journal of Infectious Diseases, . Article Number jiae472. ISSN 1537-6613. (doi:10.1093/infdis/jiae472) (KAR id:107437)

Abstract

The development of a universal influenza vaccine likely requires an understanding of previous exposure to influenza virus (through vaccination or infection) and how that shapes the antibody repertoire to vaccination, sometimes called Original Antigenic Sin or antigenic imprinting. Whilst animal models can have a much more defined exposure history, they lack a human B cell repertoire. Transgenic mice with the complete human immunoglobulin locus enable studies of controlled infection history leading to human-like antibody evolution. Here we evaluated responses to influenza in the Intelliselect Transgenic mouse (the Kymouse). We show the Kymouse is susceptible to disease following infection with either H1N1, H3N2 or B/Yam influenza viruses and that it induces a robust binding and neutralising antibody response to all three strains of influenza virus. This study demonstrates that human B cell repertoire mice can be used for influenza virus studies, providing a tool for further interrogation of the antibody response.

Item Type: Article
DOI/Identification number: 10.1093/infdis/jiae472
Uncontrolled keywords: influenza, antibody, humanized, antigenic sin, universal vaccine
Subjects: R Medicine > RA Public aspects of medicine
Divisions: Divisions > Division of Natural Sciences > Medway School of Pharmacy
Funders: University of Kent (https://ror.org/00xkeyj56)
SWORD Depositor: JISC Publications Router
Depositing User: JISC Publications Router
Date Deposited: 18 Oct 2024 11:35 UTC
Last Modified: 15 Nov 2024 11:02 UTC
Resource URI: https://kar.kent.ac.uk/id/eprint/107437 (The current URI for this page, for reference purposes)

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