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Review
. 2012;32(1):65-79.
doi: 10.1615/critrevimmunol.v32.i1.40.

Regulation generation: the suppressive functions of human regulatory T cells

Wendy A Goodman  1 Kevin D CooperThomas S McCormick
Affiliations
Review

Regulation generation: the suppressive functions of human regulatory T cells

Wendy A Goodman et al. Crit Rev Immunol. 2012.

Abstract

Proper regulation of immune homeostasis is necessary to limit inflammation and prevent autoimmune and chronic inflammatory diseases. Many autoimmune diseases, such as psoriasis, are driven by vicious cycles of activated T cells that are unable to be suppressed by regulatory T cells. Effective suppression of auto-reactive T cells by regulatory T cells (Treg) is critical for the prevention of spontaneous autoimmune disease. Psoriatic Treg cells have been observed to a defect in their capacity to regulate, which clearly contributes to psoriasis pathogenesis. A challenge for translational research is the development of novel therapeutic interventions for autoimmune diseases that will result in durable remissions. Understanding the mechanism(s) of dysregulated T cell responses in autoimmune disease will allow for the development of future therapeutic strategies that may be employed to specifically target pathogenic, proinflammatory cells. Several reports have demonstrated a pathogenic role for Thl and Thl7 cells in psoriasis as well as other autoimmune diseases. Similarly, several laboratories have independently demonstrated functional defects in regulatory T cells isolated from patients with numerous divergent autoimmune diseases. One primary challenge of research in autoimmune diseases is therefore to restore the balance between chronic T cell activation and impairment of Treg suppressor mechanisms. To this end, it is critical to develop an understanding of the many suppressive mechanisms employed by Treg cells in hopes of developing more targeted therapeutic strategies for Treg-mediated autoimmune diseases.

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Figures

Figure 1
Figure 1
Human regulatory T cells use several diverse mechanisms to maintain immune tolerance. Shown in the figure are functional mechanisms used by human Treg cells to maintain suppression of target cells. Mechanisms include the release of secreted cytokines, such as TGFβ, IL-10 and IL-35; cytolysis of target cells; generation of immunosuppressive adenosine; and effects on dendritic cell co-stimulation.
See this image and copyright information in PMC

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