TIMs: central regulators of immune responses

Hafler, David A.; Kuchroo, Vijay K.

doi:10.1083/jcb1835oia12

Cited by 10 publications

(20 citation statements)

References 7 publications

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“…Although the expression of PD-1 has been associated with T-cell exhaustion in HIV, HCV, and lymphocytic choriomeningitis virus (12,14), not all exhausted T cells express PD-1, supporting the concept that other inhibitory molecules are likely involved. The Tim family of genes, comprising eight members in mice and three members in humans, are located in regions associated with autoimmune and allergic diseases (9,23). Tim molecules are expressed on T cells, monocytes, and antigen-presenting cells, including macrophages and dendritic cells (9).…”

Section: Discussionmentioning

confidence: 99%

“…The Tim family of genes, comprising eight members in mice and three members in humans, are located in regions associated with autoimmune and allergic diseases (9,23). Tim molecules are expressed on T cells, monocytes, and antigen-presenting cells, including macrophages and dendritic cells (9). Tim-3 was initially found to be expressed on Th1 but not Th2 cells in mice (23), and reduction of Tim-3 expression in T cells using small interfering RNA or blocking antibodies was shown to increase secretion of the antiviral cytokine IFN-␥.…”

Section: Discussionmentioning

confidence: 99%

“…Recently, upregulation of programmed death 1 (PD-1) and downmodulation of CD127 (interleukin-7 receptor) have been linked to functional exhaustion of T cells in chronic HCV infection (5-7, 15, 21, 22). However, not all exhausted T cells express these phenotypic changes, and blockade of the PD-1/PD-L1 signaling pathway does not always reconstitute Th1/Tc1 cytokine production (4,5), indicating that other molecules may contribute to the exhaustion typically associated with chronic viral infections (9). One such molecule is Tim-3 (T-cell immunoglobulin and mucin domain-containing molecule 3), a membrane protein initially identified on terminally differentiated Th1 but not Th2 cells in mice (9).…”

mentioning

confidence: 99%

“…However, not all exhausted T cells express these phenotypic changes, and blockade of the PD-1/PD-L1 signaling pathway does not always reconstitute Th1/Tc1 cytokine production (4,5), indicating that other molecules may contribute to the exhaustion typically associated with chronic viral infections (9). One such molecule is Tim-3 (T-cell immunoglobulin and mucin domain-containing molecule 3), a membrane protein initially identified on terminally differentiated Th1 but not Th2 cells in mice (9). A recent analysis of human immunodeficiency virus (HIV) infection demonstrates that Tim-3 is upregulated on both CD4 ϩ and CD8 ϩ T cells from patients with chronic infection relative to uninfected individuals and that virus-specific cells expressing high levels of Tim-3 secrete less IFN-␥ than do Tim-3-negative cells (10).…”

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Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 ⁺ and CD8 ⁺ T Cells

Golden–Mason

Palmer

Kassam

et al. 2009

J Virol

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A number of emerging molecules and pathways have been implicated in mediating the T-cell exhaustion characteristic of chronic viral infection. Not all dysfunctional T cells express PD-1, nor are they all rescued by blockade of the PD-1/PD-1 ligand pathway. In this study, we characterize the expression of T-cell immunoglobulin and mucin domain-containing protein 3 (Tim-3) in chronic hepatitis C infection. For the first time, we found that Tim-3 expression is increased on CD4 ؉ and CD8 ؉ T cells in chronic hepatitis C virus (HCV) infection. The proportion of dually PD-1/Tim-3-expressing cells is greatest in liver-resident T cells, significantly more so in HCV-specific than in cytomegalovirus-specific cytotoxic T lymphocytes. Tim-3 expression correlates with a dysfunctional and senescent phenotype (CD127 low CD57 high ), a central rather than effector memory profile (CD45RA negative CCR7 high ), and reduced Th1/Tc1 cytokine production. We also demonstrate the ability to enhance T-cell proliferation and gamma interferon production in response to HCV-specific antigens by blocking the Tim-3-Tim-3 ligand interaction. These findings have implications for the development of novel immunotherapeutic approaches to this common viral infection.Hepatitis C virus (HCV) is a major causative agent of chronic hepatitis, affecting approximately 200 million people throughout the world; the majority of individuals exposed to HCV become persistently infected (19). A broad array of functional impairments of virus-specific T cells from early to chronic stages of infection, including exhaustion (decreased antiviral cytokine production, cytotoxicity, and proliferative capacity) (8, 24) and arrested stages of differentiation (1, 13), is supported by considerable evidence. Recently, upregulation of programmed death 1 (PD-1) and downmodulation of CD127 (interleukin-7 [IL-7] receptor) have been linked to functional exhaustion of T cells in chronic HCV infection (5-7, 15, 21, 22). However, not all exhausted T cells express these phenotypic changes, and blockade of the PD-1/PD-L1 signaling pathway does not always reconstitute Th1/Tc1 cytokine production (4, 5), indicating that other molecules may contribute to the exhaustion typically associated with chronic viral infections (9). One such molecule is Tim-3 (T-cell immunoglobulin and mucin domain-containing molecule 3), a membrane protein initially identified on terminally differentiated Th1 but not Th2 cells in mice (9). A recent analysis of human immunodeficiency virus (HIV) infection demonstrates that Tim-3 is upregulated on both CD4 ϩ and CD8 ϩ T cells from patients with chronic infection relative to uninfected individuals and that virus-specific cells expressing high levels of Tim-3 secrete less IFN-␥ than do Tim-3-negative cells (10). In light of these findings, for the first time, this study assessed the expression of Tim-3 in chronic HCV infection. We found a higher frequency of Tim3-expressing CD4 ϩ and CD8 ϩ T cells in chronic HCV infection, with the highest on HCV-specific cytotoxic T...

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 ⁺ and CD8 ⁺ T Cells

Golden–Mason

Palmer

Kassam

et al. 2009

J Virol

Self Cite

382

378

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“…nonetheless, a few other studies have suggested that TiM-3 also can promote a proinflammatory response and antitumor immune response [85][86][87]. TiM-3 is also characterized as a key regulator of the dysfunctional CD8  T-cell phenotype [73,88].…”

Section: Expression and Inhibitory Role In Immune Response Of Tim-3mentioning

confidence: 99%

Emerging immune checkpoints for cancer therapy

Zheng

et al. 2015

Acta Oncologica

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background. Immunotherapy with immune checkpoint inhibitors has emerged as promising treatment modality for cancer based on the success of anti-CTLA-4 and -PD-1/PD-L1 antibodies. LAG-3 and TIM-3 are two new immune checkpoints. The aim of this work is to review the role and application of LAG-3 and TIM-3 for cancer immunotherapy. Material and methods. Literatures were searched and collected in Medline/PubMed. results. LAG-3 is presented as a CD4 homolog type I transmembrane protein which binds MHC class II molecules. LAG-3 negatively regulates T cell proliferation, homeostasis and function. IMP321 is formed of an extracellular portion of human LAG-3 fused to the Fc fraction of human IgG1 and has shown increased T cell responses and tolerability in phase I studies on advanced renal cell cancer. When combined with paclitaxel, IMP321 has exerted immune enhancement and tumor inhibition with no significant IMP321-related adverse events. TIM-3 belongs to the TIM family and mainly negatively regulates Th1 immunity. The TIM-3/galectin-9 pathway contributes to the suppressive tumor microenvironment. TIM-3 overexpression is associated with poor prognosis in a variety of cancers. Both LAG-3 and TIM-3 are coexpressed with other immune checkpoints. The application of LAG-3 or TIM-3 does play an important role in anti-tumor responses, and maybe better when combing with anti-CTLA-4 and anti-PD-1/L1 antibodies. conclusions. These two immune checkpoints play crucial roles in cancer development and may be used in future clinical practice of cancer therapy.

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HCV‐infected hepatocytes drive CD4⁺CD25⁺Foxp3⁺ regulatory T‐cell development through the Tim‐3/Gal‐9 pathway

et al. 2012

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Hepatitis C virus (HCV) is remarkable at disrupting human immunity to establish chronic infection. Accumulation of regulatory T cells (Tregs) and up-regulation of inhibitory signaling pathways (such as Tim-3/Gal-9) play pivotal roles in suppressing antiviral effector T cells (Teffs) that are essential for viral clearance. While Tim-3/Gal-9 interactions have been shown to negatively regulate Teffs, their role in regulating Tregs is poorly understood. To explore how Tim-3/Gal-9 interactions regulate HCV-mediated Treg development, in this study we provide pilot data showing that HCV-infected hepatocytes express higher levels of Gal-9 and TGF-β, and up-regulate Tim-3 expression and regulatory cytokines TGF-β/IL-10 in co-cultured CD4+ T cells, driving conventional CD4+ T cells into CD25+Foxp3+ Tregs. Additionally, recombinant Gal-9 protein can transform TCR-activated CD4+ T cells into Foxp3+ Tregs in a dose-dependent manner. Importantly, blocking Tim-3/Gal-9 ligations abrogates HCV-mediated Treg induction by HCV-infected hepatocytes, suggesting that Tim-3/Gal-9 interactions may regulate Foxp3+ Treg development and function during HCV infection.

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TIMs: central regulators of immune responses

Cited by 10 publications

References 7 publications

Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 ⁺ and CD8 ⁺ T Cells

Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 ⁺ and CD8 ⁺ T Cells

Emerging immune checkpoints for cancer therapy

HCV‐infected hepatocytes drive CD4⁺CD25⁺Foxp3⁺ regulatory T‐cell development through the Tim‐3/Gal‐9 pathway

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TIMs: central regulators of immune responses

Cited by 10 publications

References 7 publications

Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 + and CD8 + T Cells

Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 + and CD8 + T Cells

Emerging immune checkpoints for cancer therapy

HCV‐infected hepatocytes drive CD4+CD25+Foxp3+ regulatory T‐cell development through the Tim‐3/Gal‐9 pathway

Contact Info

Product

Resources

About

Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 ⁺ and CD8 ⁺ T Cells

Negative Immune Regulator Tim-3 Is Overexpressed on T Cells in Hepatitis C Virus Infection and Its Blockade Rescues Dysfunctional CD4 ⁺ and CD8 ⁺ T Cells

HCV‐infected hepatocytes drive CD4⁺CD25⁺Foxp3⁺ regulatory T‐cell development through the Tim‐3/Gal‐9 pathway