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Article Dans Une Revue PLoS Computational Biology Année : 2015

Within-host stochastic emergence dynamics of immune-escape mutants

Matthew Hartfield
  • Fonction : Auteur
Samuel Alizon

Résumé

Predicting the emergence of new pathogenic strains is a key goal of evolutionary epidemiology. However, the majority of existing studies have focussed on emergence at the population level, and not within a host. In particular, the coexistence of pre-existing and mutated strains triggers a heightened immune response due to the larger total pathogen population; this feedback can smother mutated strains before they reach an ample size and establish. Here, we extend previous work for measuring emergence probabilities in non-equilibrium populations, to within-host models of acute infections. We create a mathematical model to investigate the emergence probability of a fitter strain if it mutates from a self-limiting strain that is guaranteed to go extinct in the long-term. We show that ongoing immune cell proliferation during the initial stages of infection causes a drastic reduction in the probability of emergence of mutated strains; we further outline how this effect can be accurately measured. Further analysis of the model shows that, in the short-term, mutant strains that enlarge their replication rate due to evolving an increased growth rate are more favoured than strains that suffer a lower immune-mediated death rate ('immune tolerance'), as the latter does not completely evade ongoing immune proliferation due to inter-parasitic competition. We end by discussing the model in relation to within-host evolution of human pathogens (including HIV, hepatitis C virus, and cancer), and how ongoing immune growth can affect their evolutionary dynamics.
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Dates et versions

hal-01567908 , version 1 (05-05-2018)

Identifiants

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Matthew Hartfield, Samuel Alizon. Within-host stochastic emergence dynamics of immune-escape mutants. PLoS Computational Biology, 2015, 11 (3), pp.e1004149. ⟨10.1371/journal.pcbi.1004149⟩. ⟨hal-01567908⟩
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