Synergistic Reversal of Intrahepatic HCV-Specific CD8 T Cell Exhaustion by Combined PD-1/CTLA-4 Blockade

Nakamoto, Nobuhiro; Cho, Hyosun; Shaked, Abraham; Olthoff, Kim M.; Valiga, Mary E.; Kaminski, Mary; Gostick, Emma; Price, David A.; Freeman, Gordon J.; Wherry, E. John; Chang, Kyong–Mi

doi:10.1371/journal.ppat.1000313

Cited by 332 publications

(334 citation statements)

References 54 publications

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“…Moreover, PD-1 blockade seems to reactivate effector T cells through the targeting of certain transcriptional factors (i.e., nuclear factor kappa-light-chainenhancer of activated B cells, interferon regulatory factors 1 and 2, orphan nuclear receptor NR4A1, and B-lymphocyte-induced maturation protein 1) that cause a reengagement of the effector mechanisms in the epigenome of exhausted T cells 59 . CTLA-4 has also been found to have a clear role in multiple chronic infections, including HBV, HCV, and HIV, and its inhibition can increase the function of pathogen-specific T cells 60,61 . Epigenetic and transcriptional mechanisms determine the functional plasticity of T cells to switch between their exhausted and effector states 62 , and so altering the transcriptional landscape-for example, by manipulating transcription-factor and gene-enhancer expression-and epigenetic landscape-for example, by manipulating the activity of histone-modifying methylation or demethylation enzymes, histone acetylases, and DNA demethylases-of adoptively transferred T cells may yield a more specific anti-tumor response than generalized PD-1 and CTLA-4 blockade.…”

Section: Autoimmune Consequencesmentioning

confidence: 99%

Is autoimmunity the Achilles' heel of cancer immunotherapy?

June

Warshauer

Bluestone

2017

Nat Med

382

308

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Section: Autoimmune Consequencesmentioning

confidence: 99%

Is autoimmunity the Achilles' heel of cancer immunotherapy?

June

Warshauer

Bluestone

2017

Nat Med

382

308

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“…PD-1 has been identified as a major cell-surface inhibitory receptor capable of regulating CD8 + and CD4 + T cell exhaustion in mice, as well as in humans and nonhuman primates (50). Tim-3 and CTLA-4 were recently found to be overexpressed on HIV-and hepatitis C virus-specific CD8 + and CD4 + T cells and to act to suppress effector functions of activated T cells (11)(12)(13)51). Upregulation of LAG-3 was also shown to correlate with the impaired effector functions and exhaustion of CD8 + T cells (10,52,53).…”

Section: Discussionmentioning

confidence: 99%

“…In addition to these inhibitory receptors, it was demonstrated that a variety of other inhibitory receptors were expressed on exhausted CD8 + T cells in chronic virus infections, and the increased levels of expression were critically associated with the severity of infection and the lower functionality of CD8 + T cells (10). Although the precise inhibitory mechanisms of each individual pathway are unclear, some inhibitory receptors, such as Tim-3, LAG-3, and CTLA4, are known to negatively regulate CD8 + T cell function cooperatively with PD-1, because combined blockade of these inhibitory receptors, along with the PD-1/PD-L1 pathway, synergistically improved CD8 + T cell responses (10)(11)(12)(13). Based on the present observations, Ag-specific effector CD8 + T cells in FV-infected mice seemed to be undergoing unusually rapid and extremely severe exhaustion.…”

Section: Discussionmentioning

confidence: 99%

“…A recent study using the lymphocytic choriomeningitis virus (LCMV) provided a likely explanation for the relatively limited effect of the PD-1 blockade: exhausted CD8 + T cells are coregulated by multiple inhibitory receptors during chronic infection (10). Thus, targeting the precise inhibitory receptors for blockade (10)(11)(12)(13), the timing and duration of treatment, and combination with additional therapeutic vaccination and/or antiviral drugs (14) must be considered to establish the optimal therapeutic strategy that can improve/restore the function of virus-specific CD8 + T cells without enhancing immunopathology.…”

mentioning

confidence: 99%

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Premature Terminal Exhaustion of Friend Virus-Specific Effector CD8+ T Cells by Rapid Induction of Multiple Inhibitory Receptors

Takamura¹,

Tsuji-Kawahara²,

Yagita

et al. 2010

The Journal of Immunology

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During chronic viral infection, persistent exposure to viral Ags leads to the overexpression of multiple inhibitory cell-surface receptors that cause CD8+ T cell exhaustion. The severity of exhaustion correlates directly with the level of infection and the number and intensity of inhibitory receptors expressed, and it correlates inversely with the ability to respond to the blockade of inhibitory pathways. Friend virus (FV) is a murine retrovirus complex that induces acute high-level viremia, followed by persistent infection and leukemia development, when inoculated into immunocompetent adult mice. In this article, we provide conclusive evidence that FV infection results in the generation of virus-specific effector CD8+ T cells that are terminally exhausted. Acute FV-induced disease is characterized by a rapid increase in the number of virus-infected erythroblasts, leading to massive splenomegaly. Most of the expanded erythroblasts strongly express programmed death ligand-1 and MHC class I, thereby creating a highly tolerogenic environment. Consequently, FV-specific effector CD8+ T cells uniformly express multiple inhibitory receptors, such as programmed cell death 1 (PD-1), T cell Ig domain and mucin domain 3 (Tim-3), lymphocyte activation gene-3, and CTLA-4, rapidly become nonresponsive to restimulation and are no longer reinvigorated by combined in vivo blockade of PD-1 and Tim-3 during the memory phase. However, combined blockade of PD-1 and Tim-3 during the priming/differentiation phase rescued FV-specific CD8+ T cells from becoming terminally exhausted, resulting in improved CD8+ T cell functionality and virus control. These results highlight FV’s unique ability to evade virus-specific CD8+ T cell responses and the importance of an early prophylactic approach for preventing terminal exhaustion of CD8+ T cells.

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“…The strongest evidence that exhausted cells retain the ability to mount a potent effector response comes from the many studies in which strong anti-tumor or anti-viral immunity could be restored by blocking PD-1/PD-L1 interaction alone or in combination with targeting other receptors [46][47][48][49][50][51][52] . This approach of antibody-mediated "checkpoint blockade" is now increasingly used to treat patients with cancer and its impact on chronic infections in humans is being evaluated (Box 1).…”

Section: Evidence That Functional T-cells Are Maintained In Chronic Imentioning

confidence: 99%

T cell differentiation in chronic infection and cancer: functional adaptation or exhaustion?

et al. 2014

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Chronic viral infections and malignant tumours induce T cells that have a reduced ability to secrete effector cytokines and have upregulated expression of the inhibitory receptor PD1 (programmed cell death protein 1). These features have so far been considered to mark terminally differentiated 'exhausted' T cells. However, several recent clinical and experimental observations indicate that phenotypically exhausted T cells can still mediate a crucial level of pathogen or tumour control. In this Opinion article, we propose that the exhausted phenotype results from a differentiation process in which T cells stably adjust their effector capacity to the needs of chronic infection. We argue that this phenotype is optimized to cause minimal tissue damage while still mediating a critical level of pathogen control. In contrast to the presently held view of functional exhaustion, this new concept better reflects the pathophysiology and clinical manifestations of persisting infections, and it provides a rationale for emerging therapies that enhance T cell activity in chronic infection and cancer by blocking inhibitory receptors. Daniel T. Utzschneider Division of Immunology and Allergy of the Lausanne University Hospital (CHUV) and Swiss Vaccine Research Institute (SVRI), Lausanne, SwitzerlandDaniel Utzschneider is a PhD student of Dietmar Zehn. His research is focused on T-cell differentiation in chronic infection. Susanne G. Oberle Division of Immunology and Allergy of the Lausanne University Hospital (CHUV) and Swiss Vaccine Research Institute (SVRI), Lausanne, SwitzerlandSusanne Oberle is a PhD student of Dietmar Zehn. Her research interests are focused on investigating T-cell responses in acute and chronic infections. and it provides a rational for emerging therapies that enhance T-cell activity in chronic infection and cancer by blocking inhibitory receptors. Christian Münz PhD

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Synergistic Reversal of Intrahepatic HCV-Specific CD8 T Cell Exhaustion by Combined PD-1/CTLA-4 Blockade

Cited by 332 publications

References 54 publications

Is autoimmunity the Achilles' heel of cancer immunotherapy?

Is autoimmunity the Achilles' heel of cancer immunotherapy?

Premature Terminal Exhaustion of Friend Virus-Specific Effector CD8+ T Cells by Rapid Induction of Multiple Inhibitory Receptors

T cell differentiation in chronic infection and cancer: functional adaptation or exhaustion?

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