Effect of PD-1

Young, John S.; Heffernan, Daithi S.; Chung, Chun‐Shiang; Kettenmann, Maude L.; Young, Whitney A.; Guillen, Valeria Sanabria; Cioffi, William G.; Ayala, Alfred

doi:10.1097/shk.0000000000000553

Cited by 16 publications

(21 citation statements)

References 34 publications

(87 reference statements)

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“…i NKT cells regulate clearance of the peritoneal bacterial septic burden and affect influx of key immune cells. Specifically, within adults, we have noted that this i NKT cell regulation of the immune response to sepsis is controlled by the regulatory checkpoint protein PD-1 ( 16 ), a finding not previously observed in neonates.…”

Section: Introductionmentioning

confidence: 52%

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Program Cell Death Receptor-1-Mediated Invariant Natural Killer T-Cell Control of Peritoneal Macrophage Modulates Survival in Neonatal Sepsis

et al. 2017

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We have shown that invariant natural killer T (iNKT) cells mediate sepsis-induced end-organ changes and immune responses, including macrophage bacterial phagocytosis, a finding regulated by the check point protein program cell death receptor-1 (PD-1). Furthermore, PD-1 mediates mortality in both adult and neonatal murine sepsis as well as in surgical patients. Given our previous findings, we hypothesize that iNKT cells will also modulate neonatal sepsis survival, and that this effect is regulated in part through PD-1. We utilized a polymicrobial intra-peritoneal cecal slurry (CS) sepsis model in wild type (WT), iNKT−/− or PD-1−/− 5–7 day old neonatal pups. Typically, tissues were harvested at 24 h for various bioassays/histology and, in some cases, survival was assessed for up to 7 days. Interestingly, similar to what we recently reported for PD-1−/− mice following CS, iNKT−/−-deficient animals exhibit a markedly improved survival vs. WT. Histologically, minor alterations in liver architectural, which were noted in WT pups, were attenuated in both iNKT−/− and PD-1−/− pups. Following CS, PECAM-1 expression was unchanged in the WT pups but increased in both iNKT−/− and PD-1−/− pups. In WT, following CS the emergence of a Ly6Clow subpopulation was noted among the influxed peritoneal macrophage population. Conversely, within iNKT−/− pups, there were fewer peritoneal macrophages and a greater percentage of Ly6Chigh macrophages. We show not only a key role for iNKT cells in affecting end-organ damage as well as alterations in phagocytes phenotypes in neonatal sepsis but that this iNKT cell mediated effect is driven by the central checkpoint protein PD-1.

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Section: Introductionmentioning

confidence: 52%

“…The CS model at our institution is modification ( 16 ) of the model previously described by Wynn et al ( 17 ). In brief, a naive WT adult donor mouse (C57BL/6J) was euthanized and cecal contents were harvested.…”

Section: Methodsmentioning

confidence: 99%

Program Cell Death Receptor-1-Mediated Invariant Natural Killer T-Cell Control of Peritoneal Macrophage Modulates Survival in Neonatal Sepsis

et al. 2017

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“…Subsequently, Wang et al (106) showed that PMNs from CLP mice and patients diagnosed with severe sepsis exhibited a substantial rise in their PD-L1 expression, correlating with increased morbidity in the septic patients. Additionally, these cells, via direct contact, were capable of inducing a marked increase in lymphocytic cell death/dysfunction (another common feature of the septic animal/patient) as well as altering the migrational functionality of the cell (a dysfunction also noted by Young et al (107) in septic mouse i NKT cells) (22). More recently, Patera et al (53) have further found that peripheral blood PMNs from septic patients that expressed high levels of PD-L1 exhibited a decline in their capacity to phagocytize bacteria, a reduction of CD168 expression and a poor production of TNF-α in response to stimuli.…”

Section: Discussionmentioning

confidence: 98%

“…i NKT-cells are capable of both a Th1 and a Th2 response and interact with a diverse array of immune cells serving to both positively and negatively regulate the immune and inflammatory response i NKT-cells are capable of trafficking both within the liver in response to a sterile injury (74), in and out the lung in response to an infection (75). As well as distally to a septic source in the abdomen (76). i NKT-cells are themselves regulated by co-inhibitory/checkpoint proteins, most notably PD-1.…”

Section: Discussionmentioning

confidence: 99%

“…Initial activation of i NKT-cells is associated with increased PD-1 expression upon i NKT-cells (77) (Figure 4, Component [2]). Young et al (76) showed that direct ligation of PD-1 with its ligand PD-L1 is essential to trafficking and migration of i NKT-cells and PD-1 is essential to regulation of chemokine receptor expression upon i NKT-cells. Conversely, repeated stimulation of PD-1 upon i NKT-cells has been shown to induce anergy (78) a mechanism that is believed to have developed to protect against an over-exuberant i NKT-cell driven immune response.…”

Section: Discussionmentioning

confidence: 99%

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A novel role for coinhibitory receptors/checkpoint proteins in the immunopathology of sepsis

Fallon

Girard

Chung

et al. 2018

Journal of Leukocyte Biology

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Coinhibitory molecules, such as PD-1, CTLA-4, 2B4, and BTLA, are an important new family of mediators in the pathophysiology of severe bacterial and/or fungal infection, as well as the combined insults of shock and sepsis. Further, the expression of these molecules may serve as indicators of the immune status of the septic individual. Using PD-1:PD-L as an example, we discuss in this review how such checkpoint molecules may affect the host response to infection by mediating the balance between effective immune defense and immune-mediated tissue injury. Additionally, we explore how the up-regulation of PD-1 and/or PD-L1 expression on not only adaptive immune cells (e.g., T cells), but also on innate immune cells (e.g., macrophages, monocytes, and neutrophils), as well as nonimmune cells during sepsis and/or shock contributes to functional alterations often with detrimental sequelae.

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The pathogenesis and potential therapeutic targets in sepsis

Zhang,

Jiang,

et al. 2023

MedComm

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Sepsis is defined as “a life‐threatening organ dysfunction caused by dysregulated host systemic inflammatory and immune response to infection.” At present, sepsis continues to pose a grave healthcare concern worldwide. Despite the use of supportive measures in treating traditional sepsis, such as intravenous fluids, vasoactive substances, and oxygen plus antibiotics to eradicate harmful pathogens, there is an ongoing increase in both the morbidity and mortality associated with sepsis during clinical interventions. Therefore, it is urgent to design specific pharmacologic agents for the treatment of sepsis and convert them into a novel targeted treatment strategy. Herein, we provide an overview of the molecular mechanisms that may be involved in sepsis, such as the inflammatory response, immune dysfunction, complement deactivation, mitochondrial damage, and endoplasmic reticulum stress. Additionally, we highlight important targets involved in sepsis‐related regulatory mechanisms, including GSDMD, HMGB1, STING, and SQSTM1, among others. We summarize the latest advancements in potential therapeutic drugs that specifically target these signaling pathways and paramount targets, covering both preclinical studies and clinical trials. In addition, this review provides a detailed description of the crosstalk and function between signaling pathways and vital targets, which provides more opportunities for the clinical development of new treatments for sepsis.

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Effect of PD-1

Cited by 16 publications

References 34 publications

Program Cell Death Receptor-1-Mediated Invariant Natural Killer T-Cell Control of Peritoneal Macrophage Modulates Survival in Neonatal Sepsis

Program Cell Death Receptor-1-Mediated Invariant Natural Killer T-Cell Control of Peritoneal Macrophage Modulates Survival in Neonatal Sepsis

A novel role for coinhibitory receptors/checkpoint proteins in the immunopathology of sepsis

The pathogenesis and potential therapeutic targets in sepsis

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