T Cell Immunity. Functional Heterogeneity of Human Memory CD4⁺ T Cell Clones Primed by Pathogens or Vaccines

Overview

Journal Science

Specialty Science

Date 2014 Dec 6

PMID 25477212

Citations 194

Authors

Simone Becattini

Daniela Latorre

Federico Mele

Mathilde Foglierini

Corinne De Gregorio

Antonino Cassotta

Blanca Fernandez

Sander Kelderman

Ton N Schumacher

Davide Corti

Antonio Lanzavecchia

Federica Sallusto

Affiliations

Soon will be listed here.

Abstract

Distinct types of CD4(+) T cells protect the host against different classes of pathogens. However, it is unclear whether a given pathogen induces a single type of polarized T cell. By combining antigenic stimulation and T cell receptor deep sequencing, we found that human pathogen- and vaccine-specific T helper 1 (T(H)1), T(H)2, and T(H)17 memory cells have different frequencies but comparable diversity and comprise not only clones polarized toward a single fate, but also clones whose progeny have acquired multiple fates. Single naïve T cells primed by a pathogen in vitro could also give rise to multiple fates. Our results unravel an unexpected degree of interclonal and intraclonal functional heterogeneity of the human T cell response and suggest that polarized responses result from preferential expansion rather than priming.

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