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Review
. 2021 Mar;51(3):512-530.
doi: 10.1002/eji.202048614. Epub 2021 Feb 19.

CD8+ Tregs revisited: A heterogeneous population with different phenotypes and properties

Veronika Niederlova  1 Oksana Tsyklauri  1   2 Tereza Chadimova  1   3 Ondrej Stepanek  1
Affiliations
Free article
Review

CD8+ Tregs revisited: A heterogeneous population with different phenotypes and properties

Veronika Niederlova et al. Eur J Immunol. 2021 Mar.
Free article

Abstract

Regulatory T cells (Tregs) play a key role in the peripheral self-tolerance and preventing autoimmunity. While classical CD4+ Foxp3+ Tregs are well established, their CD8+ counterparts are still controversial in many aspects including their phenotypic identity and their mechanisms of suppression. Because of these controversies and because of only a limited number of studies documenting the immunoregulatory function of CD8+ Tregs in vivo, the concept of CD8+ Tregs is still not unanimously accepted. We propose that any T-cell subset considered as true regulatory must be distinguishable from other cell types and must suppress in vivo immune responses via a known mechanism. In this article, we revisit the concept of CD8+ Tregs by focusing on the characterization of individual CD8+ T-cell subsets with proposed regulatory capacity separately. Therefore, we review the phenotype and function of CD8+ FOXP3+ T cells, CD8+ CD122+ T cells, CD8+ CD28low/- T cells, CD8+ CD45RClow T cells, T cells expressing CD8αα homodimer and Qa-1-restricted CD8+ T cells to show whether there is sufficient evidence to establish these subsets as bona fide Tregs. Based on the intrinsic ability of CD8+ Treg subsets to promote immune tolerance in animal models, we elaborate on their potential use in clinics.

Keywords: Autoimmunity; CD8 T cells; Homeostasis; Regulatory T cells; Tolerance.

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References

    1. Gershon, R. K. and Kondo, K., Cell interactions in the induction of tolerance: the role of thymic lymphocytes. Immunology 1970. 18: 723-737.
    1. Sakaguchi, S., Sakaguchi, N., Asano, M., Itoh, M. and Toda, M., Immunologic self-tolerance maintained by activated T cells expressing IL-2 receptor alpha-chains (CD25). Breakdown of a single mechanism of self-tolerance causes various autoimmune diseases. J. Immunol. 1995. 155: 1151-1164.
    1. Fontenot, J. D., Gavin, M. A. and Rudensky, A. Y., Foxp3 programs the development and function of CD4+CD25+ regulatory T cells. Nat. Immunol. 2003. 4: 330-336.
    1. Flippe, L., Bézie, S., Anegon, I. and Guillonneau, C., Future prospects for CD8(+) regulatory T cells in immune tolerance. Immunol. Rev. 2019. 292: 209-224.
    1. Vieyra-Lobato, M. R., Vela-Ojeda, J., Montiel-Cervantes, L., López-Santiago, R. and Moreno-Lafont, M. C., Description of CD8(+) regulatory T lymphocytes and their specific intervention in graft-versus-host and infectious diseases, autoimmunity, and cancer. J Immunol Res 2018. 2018: 1-16.

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