Quantifying T Cell Cross-Reactivity: Influenza and Coronaviruses

Author:

Gaevert Jessica AnnORCID,Luque Duque DanielORCID,Lythe GrantORCID,Molina-París CarmenORCID,Thomas Paul GlyndwrORCID

Abstract

If viral strains are sufficiently similar in their immunodominant epitopes, then populations of cross-reactive T cells may be boosted by exposure to one strain and provide protection against infection by another at a later date. This type of pre-existing immunity may be important in the adaptive immune response to influenza and to coronaviruses. Patterns of recognition of epitopes by T cell clonotypes (a set of cells sharing the same T cell receptor) are represented as edges on a bipartite network. We describe different methods of constructing bipartite networks that exhibit cross-reactivity, and the dynamics of the T cell repertoire in conditions of homeostasis, infection and re-infection. Cross-reactivity may arise simply by chance, or because immunodominant epitopes of different strains are structurally similar. We introduce a circular space of epitopes, so that T cell cross-reactivity is a quantitative measure of the overlap between clonotypes that recognize similar (that is, close in epitope space) epitopes.

Funder

National Institutes of Health

Laboratory Directed Research and Development

European Union's Horizon 2020 research and innovation program under the Marie Skłodowska-Curie

Publisher

MDPI AG

Subject

Virology,Infectious Diseases

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