An obligate cell-intrinsic function for CD28 in Tregs
Ruan Zhang, … , Jonathan S. Maltzman, Laurence A. Turka
Ruan Zhang, … , Jonathan S. Maltzman, Laurence A. Turka
Published January 2, 2013
Citation Information: J Clin Invest. 2013;123(2):580-593. https://doi.org/10.1172/JCI65013.
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Research Article Immunology

An obligate cell-intrinsic function for CD28 in Tregs

Abstract

Tregs expressing the transcription factor FOXP3 are critical for immune homeostasis. The costimulatory molecule CD28 is required for optimal activation and function of naive T cells; however, its role in Treg function has been difficult to dissect, as CD28 is required for thymic Treg development, and blockade of CD28-ligand interactions has confounding effects in trans on nonregulatory cells. To address this question, we created Treg-specific Cd28 conditional knockout mice. Despite the presence of normal numbers of FOXP3+ cells, these animals accumulated large numbers of activated T cells, developed severe autoimmunity that primarily affected the skin and lungs, and failed to appropriately resolve induced experimental allergic encephalomyelitis. This in vivo functional impairment was accompanied by dampened expression of CTLA-4, PD-1, and CCR6. Disease occurrence was not due to subversion of Cd28-deficient Tregs into pathogenic cells, as complementation with normal Tregs prevented disease occurrence. Interestingly, in these “competitive” environments, Cd28-deficient Tregs exhibited a pronounced proliferative/survival disadvantage. These data demonstrate clear postmaturational roles for CD28 in FOXP3+ Tregs and provide mechanisms which we believe to be novel to explain how interruption of CD28-ligand interactions may enhance immune responses independent of effects on thymic development or on other cell types.

Authors

Ruan Zhang, Alexandria Huynh, Gregory Whitcher, JiHoon Chang, Jonathan S. Maltzman, Laurence A. Turka

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Figure 4

Cd28-ΔTreg mice develop autoimmunity with skin inflammation.

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Cd28-ΔTreg mice develop autoimmunity with skin inflammation. (A) Gros...
(A) Gross appearance and lymph nodes and spleens from representative WT littermate control (labeled 1 and 3) and Cd28-ΔTreg (labeled 2 and 4) mice. (B) Cell numbers in lymph nodes and spleens from 2- to 5-month-old mice. 6 littermate pairs were analyzed. Data represent mean ± SEM. (C) H&E staining of skin and lung tissue in a 3-month-old Cd28-ΔTreg mouse. Original magnification, ×400. (D) CD44+CD62Lhi cells in lymph nodes of a representative 4-month-old Cd28-ΔTreg mice. (E) Proportions of CD44+ cells from lymph nodes of 2-month-old mice. 5 littermate pairs were analyzed. Data represent mean ± SEM. (F) Percentage of IFN-γ+ cells in stimulated splenocytes from 2- to 5-month-old littermate pairs. Symbols represent individual mice; horizontal bars indicate the mean.