Literature DB >> 33679715

Immune Deregulation in Sepsis and Septic Shock: Reversing Immune Paralysis by Targeting PD-1/PD-L1 Pathway.

Yuki Nakamori1, Eun Jeong Park1, Motomu Shimaoka1.   

Abstract

Sepsis remains a major problem for human health worldwide, thereby manifesting high rates of morbidity and mortality. Sepsis, once understood as a monophasic sustained hyperinflammation, is currently recognized as a dysregulated host response to infection, with both hyperinflammation and immunoparalysis occurring simultaneously from the earliest stages of sepsis, involving multiple organ dysfunctions. Despite the recent progress in the understanding of the pathophysiology underlying sepsis, no specific treatment to restore immune dysregulation in sepsis has been validated in clinical trials. In recent years, treatment for immune checkpoints such as the programmed cell death protein 1/programmed death ligand (PD-1/PD-L) pathway in tumor-infiltrating T-lymphocytes has been successful in the field of cancer immune therapy. As immune-paralysis in sepsis involves exhausted T-lymphocytes, future clinical applications of checkpoint inhibitors for sepsis are expected. In addition, the functions of PD-1/PD-L on innate lymphoid cells and the role of exosomal forms of PD-L1 warrant further research. Looking back on the history of repeatedly failed clinical trials of immune modulatory therapies for sepsis, sepsis must be recognized as a difficult disease entity for performing clinical trials. A major obstacle that could prevent effective clinical trials of drug candidates is the disease complexity and heterogeneities; clinically diagnosed sepsis could contain multiple sepsis subgroups that suffer different levels of hyper-inflammation and immune-suppression in distinct organs. Thus, the selection of appropriate more homogenous sepsis subgroup is the key for testing the clinical efficacy of experimental therapies targeting specific pathways in either hyperinflammation and/or immunoparalysis. An emerging technology such as artificial intelligence (AI) may help to identify an immune paralysis subgroup who would best be treated by PD-1/PD-L1 pathway inhibitors.
Copyright © 2021 Nakamori, Park and Shimaoka.

Entities:  

Keywords:  PD-1; PD-L; artificial intelligence; immune checkpoints inhibitors; immunomodulation; immunoparalysis; machine learning; sepsis - diagnostics

Year:  2021        PMID: 33679715      PMCID: PMC7925640          DOI: 10.3389/fimmu.2020.624279

Source DB:  PubMed          Journal:  Front Immunol        ISSN: 1664-3224            Impact factor:   7.561


  130 in total

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3.  Anti-cachectin/TNF monoclonal antibodies prevent septic shock during lethal bacteraemia.

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5.  IL-7 Restores T Lymphocyte Immunometabolic Failure in Septic Shock Patients through mTOR Activation.

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6.  Tumor necrosis factor mediates endotoxic effects in mice.

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Journal:  Infect Immun       Date:  1987-07       Impact factor: 3.441

7.  Treatment of septic shock with the tumor necrosis factor receptor:Fc fusion protein. The Soluble TNF Receptor Sepsis Study Group.

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10.  Differential Roles of Dendritic Cells in Expanding CD4 T Cells in Sepsis.

Authors:  Samuel Darkwah; Nodoka Nago; Michael G Appiah; Phyoe Kyawe Myint; Eiji Kawamoto; Motomu Shimaoka; Eun Jeong Park
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Review 2.  The Neonatal Innate Immune Response to Sepsis: Checkpoint Proteins as Novel Mediators of This Response and as Possible Therapeutic/Diagnostic Levers.

Authors:  Emily Hensler; Habesha Petros; Chyna C Gray; Chun-Shiang Chung; Alfred Ayala; Eleanor A Fallon
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3.  N6-methyladenosine (m6A) methyltransferase METTL3 regulates sepsis-induced myocardial injury through IGF2BP1/HDAC4 dependent manner.

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Review 6.  The Role of Circadian Clock Genes in Critical Illness: The Potential Role of Translational Clock Gene Therapies for Targeting Inflammation, Mitochondrial Function, and Muscle Mass in Intensive Care.

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7.  Association between glucose-to-lymphocyte ratio and in-hospital mortality in intensive care patients with sepsis: A retrospective observational study based on Medical Information Mart for Intensive Care IV.

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8.  PD-1/PD-L1 blockade abrogates a dysfunctional innate-adaptive immune axis in critical β-coronavirus disease.

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Journal:  Sci Adv       Date:  2022-09-21       Impact factor: 14.957

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