Loss of the signaling adaptor TRAF1 causes CD8+ T cell dysregulation during human and murine chronic infection

Wang, Chao; McPherson, Ann J.; Jones, R. Brad; Kawamura, Kim; Lin, Gloria H. Y.; Lang, Philipp A.; Ambagala, Thanuja; Pellegrini, Marc; Calzascia, Thomas; Aidarus, Nasra; Elford, Alisha R.; Yue, Feng Yun; Kremmer, Elisabeth; Kovacs, Colin; Benko, Erika; Tremblay, Cécile; Routy, Jean‐Pierre; Bernard, Nicole F.; Ostrowski, Mario; Ohashi, Pamela S.; Watts, Tania H.

doi:10.1084/jem.20110675

Cited by 57 publications

(85 citation statements)

References 59 publications

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“…Agonist anti-OX40 has no effect on viral load in LCMV cl 13 infection (11), and agonist anti-4-1BB had minimal therapeutic effect when administered during the chronic stage of LCMV cl 13 infection due to the loss of a key signaling adaptor, TNFR-associated factor (TRAF)1, downstream of 4-1BB, with similar findings in T cells from chronically HIV-infected donors (12). Although anti-4-1BB demonstrated efficacy when combined with IL-7, which restores TRAF1 levels (12), there is growing concern that agonist therapies targeting T cell cosignaling molecules such as 4-1BB and CD28 or soluble factors such as IL-21 may induce indiscriminate or overzealous expansion of CD8 T cells and result in immune pathology (13)(14)(15)(16)(17)(18). Therefore, it remains a significant challenge to identify a T cell costimulatory molecule that is both safe and effective in improving immune function and control of viral infections.…”

mentioning

confidence: 54%

“…In addition to self-limiting inflammation, there are also examples of ineffective therapies targeting T cell costimulatory molecules. During chronic LCMV infection in mouse or HIV infection in humans, TRAF1 is lost in virus-specific CD8 T cells so 4-1BB cannot signal, and therefore anti-4-1BB is ineffective as a therapy (12). Even when 4-1BB signaling was restored by IL-7 treatment to upregulate TRAF1, these effects were not ideal in that they resulted in an increase in the total number, but not the proportion of LCMV-specific T cells (12).…”

Section: Discussionmentioning

confidence: 99%

“…During chronic LCMV infection in mouse or HIV infection in humans, TRAF1 is lost in virus-specific CD8 T cells so 4-1BB cannot signal, and therefore anti-4-1BB is ineffective as a therapy (12). Even when 4-1BB signaling was restored by IL-7 treatment to upregulate TRAF1, these effects were not ideal in that they resulted in an increase in the total number, but not the proportion of LCMV-specific T cells (12). This may be because anti-4-1BB agonist treatment can expand bystander 4-1BB + memory T cells (16)(17)(18).…”

Section: Discussionmentioning

confidence: 99%

“…there are multiple costimulatory receptors and ligands present, and the addition of exogenous GITR costimulation is redundant and therefore does not further enhance the response. However, at later time points when coinhibitory molecules predominate and costimulatory 4-1BB is desensitized (12,44), exogenous GITR costimulation is efficacious.…”

Section: Discussionmentioning

confidence: 99%

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Anti-GITR Agonist Therapy Intrinsically Enhances CD8 T Cell Responses to Chronic Lymphocytic Choriomeningitis Virus (LCMV), Thereby Circumventing LCMV-Induced Downregulation of Costimulatory GITR Ligand on APC

Clouthier

Zhou

Watts

2014

The Journal of Immunology

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The costimulatory TNFR family member GITR can provide important survival signals for CD8 T cells. However, little is known about the regulation of this pathway during a chronic infection. In this study, we show that GITR ligand (GITRL) is maximally induced on APCs at day 2 post–lymphocytic choriomeningitis virus (LCMV) clone 13 infection, but is downregulated to below baseline levels by day 8 postinfection (p.i.), and remains so at the chronic stage of infection. At its peak, GITRL expression is highest on macrophages, with lower expression on conventional and plasmacytoid dendritic cells. GITR expression was highest on T regulatory cells but was also detected on Th1 and LCMV-specific CD8 T cells at day 8 p.i. and was maintained at low, but above baseline levels at the chronic stage of LCMV infection. As GITRL was limiting at the chronic stage of infection, we investigated the potential of therapeutic stimulation of GITR at this stage using agonistic anti-GITR Ab. Anti-GITR treatment at day 21 p.i. increased the frequency and number of LCMV-specific CD8 T cells, resulting in increased in vivo CTL activity and a concomitant decrease in viral load, despite the persistence of PD-1 expression. These effects of anti-GITR were CD8 T cell intrinsic, with no detectable effects on Th1 or T regulatory cells. In contrast to other TNFR agonists, such as anti–4-1BB, which can cause immune pathology, a single therapeutic dose of anti-GITR did not induce splenomegaly or increase serum alanine transaminase. These studies identify GITR as a promising therapeutic target for chronic infection.

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mentioning

confidence: 54%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Anti-GITR Agonist Therapy Intrinsically Enhances CD8 T Cell Responses to Chronic Lymphocytic Choriomeningitis Virus (LCMV), Thereby Circumventing LCMV-Induced Downregulation of Costimulatory GITR Ligand on APC

Clouthier

Zhou

Watts

2014

The Journal of Immunology

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“…42 In short, brain, liver, lung, spleen and kidney were collected in MEM 2% FCS and frozen at − 80°C before further analysed. Organs were homogenised and supernatant dilutions were used to infect monolayers of MC57 cells (8 × 10 5 per ml), Cells were overlayed with 2% methyl cellulose (Fluka #64620) in DME and plates were incubated at 37°C, 5% CO 2 for 48 h. Viral plaque staining was performed after fixation of the cells with 4% Formalin-PBS and permeabilization with 0.1% Triton X (FLUKA #93418) with VL-4 rat anti-LCMV monoclonal antibody (WEHI Antibody Facility, Melbourne, VIC, Australia) followed by Peroxidase-conjugated AffiniPure goat anti-rat IgG (H+L) antibodies (Jackson ImmunoResearch Laboratories, West Grove, PA, USA #112-035-003).…”

Section: Foxp3mentioning

confidence: 99%

The BCL-2 pro-survival protein A1 is dispensable for T cell homeostasis on viral infection

et al. 2017

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The physiological role of the pro-survival BCL-2 family member A1 has been debated for a long time. Strong mRNA induction in T cells on T cell receptor (TCR)-engagement suggested a major role of A1 in the survival of activated T cells. However, the investigation of the physiological roles of A1 was complicated by the quadruplication of the A1 gene locus in mice, making A1 gene targeting very difficult. Here, we used the recently generated A1−/− mouse model to examine the role of A1 in T cell immunity. We confirmed rapid and strong induction of A1 protein in response to TCR/CD3 stimulation in CD4 + as well as CD8 + T cells. Surprisingly, on infection with the acute influenza HKx31 or the lymphocytic choriomeningitis virus docile strains mice lacking A1 did not show any impairment in the expansion, survival, or effector function of cytotoxic T cells. Furthermore, the ability of A1 −/− mice to generate antigen-specific memory T cells or to provide adequate CD4-dependent help to B cells was not impaired. These results suggest functional redundancy of A1 with other pro-survival BCL-2 family members in the control of T celldependent immune responses. Cell Death and Differentiation (2017) 24, 523-533; doi:10.1038/cdd.2016.155; published online 13 January 2017On antigenic challenge, T lymphocytes need to rapidly switch from their IL-7/IL-7R-regulated naive, quiescent state 1,2 to a T cell antigen-receptor (TCR/CD3) stimulation-induced activation state. 3 In case of inappropriate stimulation of the TCR, for example, in the absence of co-receptor stimulation, this shift in the survival programme is not induced and leads to rapid T cell death. 4 Conversely, appropriately stimulated T cells expand rapidly, allowing accumulation of T cell clones expressing TCRs of high affinity for specific antigens. During this clonal expansion, BCL-2 family regulated apoptosis acts as a mechanism to remove low-affinity T cells, thereby ensuring the generation of a highly effective immune response.5 On infection clearance, most of the activated T cells are removed by apoptosis, 6 leaving only some T cells with antigen-specific high-affinity TCRs in reserve as longlived memory T cells. 7The BCL-2 family of proteins regulate apoptotic cell death, with the balance between pro-survival and pro-apoptotic family members determining whether a cell lives or dies. The expression of pro-survival BCL-2 family members is dynamically regulated during T cell activation.8 TCR/CD3 ligation leads to the downregulation of BCL-2 and induction of BCL-XL.3 Accordingly, Bcl-2 −/− mice display a loss of mature, unstimulated T cells, and the death of these cells can be prevented by TCR/CD3 stimulation.9 Interestingly, although BCL-XL is substantially upregulated on TCR/CD3 stimulation, its loss did not increase apoptosis or impair proliferation of T cells stimulated with mitogenic antibodies. 10 In contrast, MCL-1 has been shown to be a crucial pro-survival factor after T cell activation.11,12 A1 is a prosurvival BCL-2 family protein that has been proposed to be i...

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TRAF family molecules in T cells: Multiple receptors and functions

Arkee

Bishop

2019

Journal of Leukocyte Biology

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The TNFR superfamily of receptors, the major focus of the recent TNFR Superfamily Conference held in June 2019, employ the TNFR‐associated factor (TRAF) family of adaptor proteins in key aspects of their signaling pathways. Although many early studies investigated TRAF functions via exogenous overexpression in nonhematopoietic cell lines, it has subsequently become clear that whereas TRAFs share some overlap in function, each also plays unique biologic roles, that can be highly context dependent. This brief review summarizes the current state of knowledge of functions of each of the TRAF molecules that mediate important functions in T lymphocytes: TRAFs 1, 2, 3, 5, and 6. Due to our current appreciation of the contextual nature of TRAF function, our focus is upon findings made specifically in T lymphocytes. Key T cell functions for each TRAF are detailed, as well as future knowledge gaps of interest and importance.

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Loss of the signaling adaptor TRAF1 causes CD8+ T cell dysregulation during human and murine chronic infection

Abstract: Loss of intracellular TRAF1 expression correlates with CD8+ T cell exhaustion and contributes to increased viral load at the chronic stage of HIV and LCMV infection, a phenotype that can be reversed by IL-7 stimulation together with 4-1BB agonist.

Cited by 57 publications

References 59 publications

Anti-GITR Agonist Therapy Intrinsically Enhances CD8 T Cell Responses to Chronic Lymphocytic Choriomeningitis Virus (LCMV), Thereby Circumventing LCMV-Induced Downregulation of Costimulatory GITR Ligand on APC

Anti-GITR Agonist Therapy Intrinsically Enhances CD8 T Cell Responses to Chronic Lymphocytic Choriomeningitis Virus (LCMV), Thereby Circumventing LCMV-Induced Downregulation of Costimulatory GITR Ligand on APC

The BCL-2 pro-survival protein A1 is dispensable for T cell homeostasis on viral infection

TRAF family molecules in T cells: Multiple receptors and functions

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