TIGIT predominantly regulates the immune response via regulatory T cells
Sema Kurtulus, … , Vijay K. Kuchroo, Ana C. Anderson
Sema Kurtulus, … , Vijay K. Kuchroo, Ana C. Anderson
Published September 28, 2015
Citation Information: J Clin Invest. 2015;125(11):4053-4062. https://doi.org/10.1172/JCI81187.
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Research Article Immunology

TIGIT predominantly regulates the immune response via regulatory T cells

Abstract

Coinhibitory receptors are critical for the maintenance of immune homeostasis. Upregulation of these receptors on effector T cells terminates T cell responses, while their expression on Tregs promotes their suppressor function. Understanding the function of coinhibitory receptors in effector T cells and Tregs is crucial, as therapies that target coinhibitory receptors are currently at the forefront of treatment strategies for cancer and other chronic diseases. T cell Ig and ITIM domain (TIGIT) is a recently identified coinhibitory receptor that is found on the surface of a variety of lymphoid cells, and its role in immune regulation is just beginning to be elucidated. We examined TIGIT-mediated immune regulation in different murine cancer models and determined that TIGIT marks the most dysfunctional subset of CD8+ T cells in tumor tissue as well as tumor-tissue Tregs with a highly active and suppressive phenotype. We demonstrated that TIGIT signaling in Tregs directs their phenotype and that TIGIT primarily suppresses antitumor immunity via Tregs and not CD8+ T cells. Moreover, TIGIT+ Tregs upregulated expression of the coinhibitory receptor TIM-3 in tumor tissue, and TIM-3 and TIGIT synergized to suppress antitumor immune responses. Our findings provide mechanistic insight into how TIGIT regulates immune responses in chronic disease settings.

Authors

Sema Kurtulus, Kaori Sakuishi, Shin-Foong Ngiow, Nicole Joller, Dewar J. Tan, Michele W.L. Teng, Mark J. Smyth, Vijay K. Kuchroo, Ana C. Anderson

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Figure 1

TIGIT is enriched on TILs.

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TIGIT is enriched on TILs. Spleen, tumor DLNs, and TILs were harvested f...
Spleen, tumor DLNs, and TILs were harvested from WT Foxp3-GFP–KI mice (n = 5) bearing B16F10 melanoma tumors and stained with Abs against CD4, CD8, and TIGIT. (A) Left panels: representative flow cytometric data showing TIGIT expression on CD4+ and CD8+ T cells in spleen, DLNs, and TILs. Right panel: frequency ± SEM of TIGIT+ cells. ****P < 0.0001 by 1-way ANOVA and Tukey’s multiple comparisons test. (B) Left panels: representative flow cytometric data showing TIGIT expression in CD4+ FOXP3 (GFP) and CD4+ FOXP3+ (GFP+) in TILs. Right panel: frequency ± SEM of TIGIT+ FOXP3 and FOXP3+ cells. CD4+ FOXP3+ percentages within total CD4+ T cells were 32.46% ± 4.27%. Data are representative of 2 to 3 experiments. ****P < 0.0001 by 1-way ANOVA and Tukey’s multiple comparisons test comparing TIGIT+ FOXP3+ cells across the indicated tissues.