Human and Mouse CD8(+)CD25(+)FOXP3(+) Regulatory T Cells at Steady State and during Interleukin-2 Therapy.

Guillaume Churlaud,Fabien Pitoiset,Roberta Lorenzon,Michelle Rosenzwajg,Bertrand Bellier,Fadi Jebbawi,David Klatzmann

doi:10.3389/fimmu.2015.00171

Abstract

In addition to CD4+ regulatory T cells (Tregs), CD8+ suppressor T cells are emerging as an important subset of regulatory T cells. Diverse populations of CD8+ T cells with suppressive activities have been described. Among them, a small population of CD8+CD25+FOXP3+ T cells is found both in mice and humans. In contrast to thymic-derived CD4+CD25+FOXP3+ Tregs, their origin and their role in the pathophysiology of autoimmune diseases (AIDs) are less understood. We report here the number, phenotype, and function of CD8+ Tregs cells in mice and humans, at the steady state and in response to low-dose interleukin-2 (IL-2). CD8+ Tregs represent approximately 0.4 and 0.1% of peripheral blood T cells in healthy humans and mice, respectively. In mice, their frequencies are quite similar in lymph nodes (LNs) and the spleen, but two to threefold higher in Peyer patches and mesenteric LNs. CD8+ Tregs express low levels of CD127. CD8+ Tregs express more activation or proliferation markers such as CTLA-4, ICOS, and Ki-67 than other CD8+ T cells. In vitro, they suppress effector T cell proliferation as well as or even better than CD4+ Tregs. Owing to constitutive expression of CD25, CD8+ Tregs are 20- to 40-fold more sensitive to in vitro IL-2 stimulation than CD8+ effector T cells, but 2–4 times less than CD4+ Tregs. Nevertheless, low-dose IL-2 dramatically expands and activates CD8+ Tregs even more than CD4+ Tregs, in mice and humans. Further studies are warranted to fully appreciate the clinical relevance of CD8+ Tregs in AIDs and the efficacy of IL-2 treatment.

Highlights

T cell development in the thymus comprises the positive selection of functional T cells capable of supporting adaptive immunity and the elimination of highly self-reactive T cells
CD4+ Tregs and CD8+ Tregs were solely defined by the co-expression of FOXP3 and CD25
We focused our study on CD8+CD25+FOXP3+ T cells, which we call CD8+ Tregs, because they are identified based on the same markers as CD4+ Tregs

Summary

Introduction

T cell development in the thymus comprises the positive selection of functional T cells capable of supporting adaptive immunity and the elimination of highly self-reactive T cells The latter process is leaky and some autoreactive effector T cells (Teffs) escape into the periphery where they are regulated by peripheral tolerance mechanisms. The best characterized of such regulatory cell populations are the natural CD4+CD25+FOXP3+ thymic-derived regulatory T cells (CD4+ Tregs) Their major role in the maintenance of immunological self-tolerance and immune homeostasis [4, 5] is illustrated by the rapid development of autoimmune diseases (AIDs) in normal mice upon their depletion [4] and by the occurrence of severe AID, allergy, and immunopathology in humans with a mutated FOXP3 gene [6]. CD8+ Tsups are less well characterized than CD4+ Tregs

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Results

Conclusion