Enhanced Effector Function of CD8+ T Cells From Healthy Controls and HIV-Infected Patients Occurs Through Thrombin Activation of Protease-Activated Receptor 1

Hurley, Amanda; Smith, Mindy; Karpova, Tatiana S.; Hasley, Rebecca B.; Belkina, Natalya; Shaw, Stephen M.; Balenga, Nariman; Druey, Kirk M.; Nickel, Erin; Packard, Beverly Z.; Imamichi, Hiromi; Hu, Zonghui; Follmann, Dean; McNally, James G.; Higgins, Jeanette; Sneller, Michael C.; Lane, H. Clifford; Catálfamo, Marta

doi:10.1093/infdis/jis730

Cited by 38 publications

(48 citation statements)

References 46 publications

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“…Less is known about the effects of PAR-1 activation on adaptive immune cells. We found that treatment with thrombin induces dose-dependent PAR-1 internalization in CD8 + T cells and confirmed an earlier report that thrombin augments IFN-γ production in purified CD8 + T cells in vitro [20]. This effect was also seen with the PAR-1 agonist TFLLR and could be blocked in both cases with the PAR-1 antagonist vorapaxar.…”

Section: Discussionsupporting

confidence: 91%

“…Consistent with the findings of Catalfamo et al [20], there was a small but significant increase in the percentage of CCR7 neg CD8 + T cells that exhibited IFN-γ production in the presence of thrombin ( Figure 5A), and the enhancement could be blocked with vorapaxar. Surprisingly, when we repeated the stimulation experiments with unseparated PBMC preparations, we observed an neg CD8 + T cells expressing IFN-γ in PBMC cultures after stimulation with anti-CD3/anti-CD28 for 6 hours in the absence (0 U/mL) or presence (0.5 U/mL) of thrombin (n = 9; right).…”

Section: T Cells With Thrombin Induced Par-1 Internalization On Cx3cr1supporting

confidence: 91%

“…Circulating immune cells can interact with soluble coagulation elements through expression of the thrombin receptor PAR-1. A recent report found increased surface PAR-1 expression on CD8 + T cells in viremic HIV-infected patients but not patients receiving ART [20]. Here we show that even among aviremic HIV-infected persons, PAR-1 surface expression is increased on all CD8 + T cells and is particularly elevated on CD8 + T cells expressing CX3CR1.…”

Section: Discussionsupporting

confidence: 55%

“…In addition to promoting clot formation, thrombin can also cleave an extracellular portion of protease-activated receptor 1 (PAR-1), subsequently activating the receptor through the newly generated N-terminus [19]. PAR-1 is expressed on the surface of CD8 + T cells as well as on monocytes, platelets, and endothelial cells [20][21][22]. A recent report indicated that PAR-1 expression is increased on the surface of CD8 + T cells from treated HIVinfected patients and that PAR-1 activation directly increases CD8 + T-cell effector function [20].…”

Section: Human Immunodeficiency Virus (Hiv) Infection Results In a Mamentioning

confidence: 99%

“…PAR-1 is expressed on the surface of CD8 + T cells as well as on monocytes, platelets, and endothelial cells [20][21][22]. A recent report indicated that PAR-1 expression is increased on the surface of CD8 + T cells from treated HIVinfected patients and that PAR-1 activation directly increases CD8 + T-cell effector function [20].…”

Section: Human Immunodeficiency Virus (Hiv) Infection Results In a Mamentioning

confidence: 99%

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Inflammatory Function of CX3CR1⁺CD8⁺T Cells in Treated HIV Infection Is Modulated by Platelet Interactions

et al. 2016

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Increases in inflammation, coagulation, and CD8 + T-cell numbers are associated with an elevated cardiovascular disease (CVD) risk in human immunodeficiency virus (HIV)-infected antiretroviral therapy (ART) recipients. Circulating memory CD8 + T cells that express the vascular endothelium-homing receptor CX3CR1 (fractalkine receptor) are enriched in HIV-infected ART recipients. Thrombin-activated receptor (PAR-1) expression is increased in HIV-infected ART recipients and is particularly elevated on CX3CR1 + CD8 + T cells, suggesting that these cells could interact with coagulation elements. Indeed, thrombin directly enhanced T-cell receptor-mediated interferon γ production by purified CD8 + T cells but was attenuated by thrombin-induced release of transforming growth factor β by platelets. We have therefore identified a population of circulating memory CD8 + T cells in HIV infection that may home to endothelium, can be activated by clot-forming elements, and are susceptible to platelet-mediated regulation. Complex interactions between inflammatory elements and coagulation at endothelial surfaces may play an important role in CVD risk in HIV-infected ART recipients.

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Section: Discussionsupporting

confidence: 91%

Section: T Cells With Thrombin Induced Par-1 Internalization On Cx3cr1supporting

confidence: 91%

Section: Discussionsupporting

confidence: 55%

Section: Human Immunodeficiency Virus (Hiv) Infection Results In a Mamentioning

confidence: 99%

Section: Human Immunodeficiency Virus (Hiv) Infection Results In a Mamentioning

confidence: 99%

See 3 more Smart Citations

Inflammatory Function of CX3CR1⁺CD8⁺T Cells in Treated HIV Infection Is Modulated by Platelet Interactions

et al. 2016

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The coagulation system in host defense

Antoniak

2018

Research and Practice in Thrombosis and Haemostasis

153

109

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The blood coagulation system and immune system of higher organisms are thought to have a common ancestral origin. During infections, the blood coagulation system is activated and components of the hemostatic system are directly involved in the immune response and immune system modulations. The current view is that the activation of coagulation is beneficial for infections with bacteria and viruses. It limits pathogen dissemination and supports pathogen killing and tissue repair. On the other hand, over‐activation can lead to thrombosis with subsequent depletion of hemostatic factors and secondary bleeding. This review will summarize the current knowledge on blood coagulation and pathogen infection with focus on most recent studies of the role of the different parts of the blood coagulation system in selected bacterial and viral infections.

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Hemostasis and tumor immunity

Cantrell

Palumbo

2022

Research and Practice in Thrombosis and Haemostasis

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Significant data have accumulated demonstrating a reciprocal relationship between cancer and the hemostatic system whereby cancer promotes life‐threatening hemostatic system dysregulation (e.g., thromboembolism, consumptive coagulopathy), and hemostatic system components directly contribute to cancer pathogenesis. The mechanistic underpinnings of this relationship continue to be defined, but it is becoming increasingly clear that many of these mechanisms involve crosstalk between the hemostatic and immune systems. This is perhaps not surprising given that there is ample evidence for bidirectional crosstalk between the hemostatic and immune systems at multiple levels that likely evolved to coordinate the response to injury, host defense, and tissue repair. Much of the data linking hemostasis and immunity in cancer biology focus on innate immune system components. However, the advent of adaptive immunity‐based cancer therapies such as immune checkpoint inhibitors has revealed that the relationship of hemostasis and immunity in cancer extends to the adaptive immune system. Adaptive immunity‐based cancer therapies appear to be associated with an increased risk of thromboembolic complications, and hemostatic system components appear to regulate adaptive immune functions through diverse mechanisms to affect tumor progression. In this review, the evidence for crosstalk between hemostatic and adaptive immune system components is discussed, and the implications of this relationship in the context of cancer therapy are reviewed. A better understanding of these relationships will likely lead to strategies to make existing adaptive immune based therapies safer by decreasing thromboembolic risk and may also lead to novel targets to improve adaptive immune‐based cancer treatments.

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Enhanced Effector Function of CD8+ T Cells From Healthy Controls and HIV-Infected Patients Occurs Through Thrombin Activation of Protease-Activated Receptor 1

Cited by 38 publications

References 46 publications

Inflammatory Function of CX3CR1⁺CD8⁺T Cells in Treated HIV Infection Is Modulated by Platelet Interactions

Inflammatory Function of CX3CR1⁺CD8⁺T Cells in Treated HIV Infection Is Modulated by Platelet Interactions

The coagulation system in host defense

Hemostasis and tumor immunity

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Enhanced Effector Function of CD8+ T Cells From Healthy Controls and HIV-Infected Patients Occurs Through Thrombin Activation of Protease-Activated Receptor 1

Cited by 38 publications

References 46 publications

Inflammatory Function of CX3CR1+CD8+T Cells in Treated HIV Infection Is Modulated by Platelet Interactions

Inflammatory Function of CX3CR1+CD8+T Cells in Treated HIV Infection Is Modulated by Platelet Interactions

The coagulation system in host defense

Hemostasis and tumor immunity

Contact Info

Product

Resources

About

Inflammatory Function of CX3CR1⁺CD8⁺T Cells in Treated HIV Infection Is Modulated by Platelet Interactions

Inflammatory Function of CX3CR1⁺CD8⁺T Cells in Treated HIV Infection Is Modulated by Platelet Interactions