Inferring the T cell repertoire dynamics of healthy individuals

Author:

Bensouda Koraichi Meriem1,Ferri Silvia12,Walczak Aleksandra M.1ORCID,Mora Thierry1

Affiliation:

1. Laboratoire de physique de l’École normale supérieure, CNRS, Paris Sciences & Lettres (PSL) University, Sorbonne Université, and Université Paris Cité, Paris 75005, France

2. Dipartimento di Fisica e Astronomia dell’Università di Bologna, Bologna 40126, Italy

Abstract

The adaptive immune system is a diverse ecosystem that responds to pathogens by selecting cells with specific receptors. While clonal expansion in response to particular immune challenges has been extensively studied, we do not know the neutral dynamics that drive the immune system in the absence of strong stimuli. Here, we learn the parameters that underlie the clonal dynamics of the T cell repertoire in healthy individuals of different ages, by applying Bayesian inference to longitudinal immune repertoire sequencing (RepSeq) data. Quantifying the experimental noise accurately for a given RepSeq technique allows us to disentangle real changes in clonal frequencies from noise. We find that the data are consistent with clone sizes following a geometric Brownian motion and show that its predicted steady state is in quantitative agreement with the observed power-law behavior of the clone-size distribution. The inferred turnover time scale of the repertoire increases with patient age and depends on the clone size in some individuals.

Funder

EC | European Research Council

Agence Nationale de la Recherche

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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