Your search keyword '"TLR3 agonist"' showing total 5 results

1. Intra-Tumoral Activation of Endosomal TLR Pathways Reveals a Distinct Role for TLR3 Agonist Dependent Type-1 Interferons in Shaping the Tumor Immune Microenvironment

Author

Kenneth G. Geles, Graham D. Thomas, Joseph Katakowski, Xiao Wang, Shobha Potluri, Shahram Salek-Ardakani, Purnima Sundar, Cecilia Oderup, Wenjing Yang, and Luca Micci

Subjects

0301 basic medicine, Agonist, Cancer Research, tumor, medicine.drug_class, medicine.medical_treatment, Antigen presentation, chemical and pharmacologic phenomena, IFN - interferon, 03 medical and health sciences, 0302 clinical medicine, Immune system, Cancer immunotherapy, Interferon, TLR9 agonist, medicine, TLR7 agonist, RC254-282, Original Research, Tumor microenvironment, Chemistry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, FOXP3, virus diseases, TLR - toll-like receptor, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, TLR3, scRNA-Seq, Cancer research, TLR3 agonist, medicine.drug

Abstract

Toll-like receptor (TLR) agonists have received considerable attention as therapeutic targets for cancer immunotherapy owing to their ability to convert immunosuppressive tumor microenvironments towards a more T-cell inflamed phenotype. However, TLRs differ in their cell expression profiles and intracellular signaling pathways, raising the possibility that distinct TLRs differentially influence the tumor immune microenvironment. Using single-cell RNA-sequencing, we address this by comparing the tumor immune composition of B16F10 melanoma following treatment with agonists of TLR3, TLR7, and TLR9. Marked differences are observed between treatments, including decreased tumor-associated macrophages upon TLR7 agonist treatment. A biased type-1 interferon signature is elicited upon TLR3 agonist treatment as opposed to a type-2 interferon signature with TLR9 agonists. TLR3 stimulation was associated with increased macrophage antigen presentation gene expression and decreased expression of PD-L1 and the inhibitory receptors Pirb and Pilra on infiltrating monocytes. Furthermore, in contrast to TLR7 and TLR9 agonists, TLR3 stimulation ablated FoxP3 positive CD4 T cells and elicited a distinct CD8 T cell activation phenotype highlighting the potential for distinct synergies between TLR agonists and combination therapy agents.

Published

2021

2. Priming With Toll-Like Receptor 3 Agonist Poly(I:C) Enhances Content of Innate Immune Defense Proteins but Not MicroRNAs in Human Mesenchymal Stem Cell-Derived Extracellular Vesicles

Author

Lisa M. Pierce and Wendy E. Kurata

Subjects

Toll-like receptor, mesenchymal stem cells, Innate immune system, Chemistry, QH301-705.5, Antimicrobial peptides, Cell Biology, Brief Research Report, Cell biology, host defense proteins, Cell and Developmental Biology, Immune system, Endopeptidase activity, TLR3, TLR3 agonist, Signal transduction, Biology (General), extracellular vesicles, priming, Defensin, poly(I:C), innate immunity, Developmental Biology, miRNA

Abstract

Mesenchymal stem cells (MSCs) help fight infection by promoting direct bacterial killing or indirectly by modulating the acute phase response, thereby decreasing tissue injury. Recent evidence suggests that extracellular vesicles (EVs) released from MSCs retain antimicrobial characteristics that may be enhanced by pretreatment of parent MSCs with the toll-like receptor 3 (TLR3) agonist poly(I:C). Our aim was to determine whether poly(I:C) priming can modify EV content of miRNAs and/or proteins to gain insight into the molecular mechanisms of their enhanced antimicrobial function. Human bone marrow-derived MSCs were cultured with or without 1 μg/ml poly(I:C) for 1 h and then conditioned media was collected after 64 h of culture in EV-depleted media. Mass spectrometry and small RNA next-generation sequencing were performed to compare proteomic and miRNA profiles. Poly(I:C) priming resulted in 49 upregulated EV proteins, with 21 known to be important in host defense and innate immunity. In contrast, EV miRNA content was not significantly altered. Functional annotation clustering analysis revealed enrichment in biological processes and pathways including negative regulation of endopeptidase activity, acute phase, complement and coagulation cascades, innate immunity, immune response, and Staphylococcus aureus infection. Several antimicrobial peptides identified in EVs remained unaltered by poly(I:C) priming, including dermcidin, lactoferrin, lipocalin 1, lysozyme C, neutrophil defensin 1, S100A7 (psoriasin), S100A8/A9 (calprotectin), and histone H4. Although TLR3 activation of MSCs improves the proteomic profile of EVs, further investigation is needed to determine the relative importance of particular functional EV proteins and their activated signaling pathways following EV interaction with immune cells.

Published

2021

3. The TLR3 Agonist Poly Inosinic:Cytidylic Acid Significantly Augments the Therapeutic Activity of an Anti-CD7 Immunotoxin for Human T-cell Leukaemia

Author

David J. Flavell, Suzanne E. Holmes, Sopsamorn U. Flavell, and Sarah L. Warnes

Subjects

0301 basic medicine, Interleukin 2, Saporin, Population, Medicine (miscellaneous), General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Immunotoxin, augmentation, Splenocyte, medicine, SCID mouse, education, lcsh:QH301-705.5, Antibody-dependent cell-mediated cytotoxicity, education.field_of_study, therapy, biology, Chemistry, CD7, Molecular biology, immunotoxin, 030104 developmental biology, Perforin, Granzyme, lcsh:Biology (General), 030220 oncology & carcinogenesis, biology.protein, TLR3 agonist, T-ALL, medicine.drug

Abstract

We have previously shown that antibody-dependent cellular cytotoxicity (ADCC) cooperates with immunotoxin (IT)-mediated killing of human leukaemia cells in an severe combined immunodeficient (SCID) mouse model of human T-cell acute lymphoblastic leukaemia (SCID-HSB-2 mice), but not in an equivalent non-obese diabetic (NOD)/SCID mouse model. In these earlier studies, we reasoned that diminished ADCC due to the functional deficit in natural killer (NK) cell activity in NOD/SCID mice resulted in a failure of effective perforin/granzyme-mediated cytotoxicity necessary for the delivery of the augmentative effect. Poly-inosinic-cytidylic acid [poly (I:C)] is a synthetic dsRNA toll-like receptor 3 (TLR3) agonist that possesses a number of biological properties that includes the in vivo activation of NK cells. We show here that intravenous (i.v.) injection of SCID mice with [poly (I:C)] results in characteristic time-related changes in serum interleukin 2 (IL-2), IL-12, and interferon &gamma, (INF&gamma, ) cytokine levels that are consistent with TLR3 driven activation of SCID mouse NK cells. Concomitantly, there are changes in the expression levels of CD2, CD16/32 (Fc&gamma, RII/RIII), CD161 (NK1.1), and F4/80 in the bulk splenocyte population. These observed changes correlate with an increase in the in vitro lytic capabilities of putative NK cells from within the splenocyte population of [poly (I:C)] treated SCID mice. We demonstrate that the in vivo activation of NK cells with [poly (I:C)] in SCID mice bearing disseminated human T-cell leukaemia xenografts resulted in a significant improvement in the therapeutic activity exerted by an intact murine monoclonal antibody against human CD7. This was also seen for a saporin-based immunotoxin constructed with the same intact antibody (HB2-SAPORIN), but not with an F(ab&rsquo, )2 derivative of the same antibody or of an IT constructed with the same F(ab&rsquo, )2 HB2 antibody derivative. This study further demonstrates the previously reported reinforcing role of ADCC for the therapeutic activity of IT in an SCID mouse model of human T-ALL and the potential to significantly boost this further with [poly (I:C)]. Our study provides the rationale to justify the exploration of the clinical utility of IT based therapeutics in combination with TLR3 agonists, such as [poly (I:C)], for the treatment of haematological, and possibly other, malignancies.

Published

2019

4. CD14+ CD15- HLA-DR- myeloid-derived suppressor cells impair antimicrobial responses in patients with acute-on-chronic liver failure

Author

Bernsmeier, C, Triantafyllou, E, Brenig, R, Lebosse, F, Singanayagam, A, Patel, V, Pop, O, Khamri, W, Nathwani, R, Tidswell, R, Weston, C, Adams, D, Thursz, M, Wendon, J, Antoniades, C, Stoneygate Trust, Medical Research Council (MRC), Wellcome Trust, Imperial College Healthcare NHS Trust- BRC Funding, and Rosetrees Trust

Subjects

Adult, MDSC, Lipopolysaccharide Receptors, Lewis X Antigen, PERIPHERAL-BLOOD, Lymphocyte Activation, THERAPY, Polymerase Chain Reaction, INCREASE, Immunophenotyping, ACTIVATION, Anti-Infective Agents, Phagocytosis, ACLF, Immune Tolerance, Humans, INNATE IMMUNE-RESPONSES, CIRRHOSIS, MONONUCLEAR-CELLS, Science & Technology, Gastroenterology & Hepatology, TRANSPLANTATION, Myeloid-Derived Suppressor Cells, bacterial infection, Acute-On-Chronic Liver Failure, 1103 Clinical Sciences, HLA-DR Antigens, Middle Aged, Flow Cytometry, Fucosyltransferases, Prognosis, TLR3 AGONIST, ALF, Cytokines, 1114 Paediatrics and Reproductive Medicine, HEPATOCELLULAR-CARCINOMA PATIENTS, immune suppression, Life Sciences & Biomedicine

Abstract

OBJECTIVE: Immune paresis in patients with acute-on-chronic liver failure (ACLF) accounts for infection susceptibility and increased mortality. Immunosuppressive mononuclear CD14+HLA-DR- myeloid-derived suppressor cells (M-MDSCs) have recently been identified to quell antimicrobial responses in immune-mediated diseases. We sought to delineate the function and derivation of M-MDSC in patients with ACLF, and explore potential targets to augment antimicrobial responses. DESIGN: Patients with ACLF (n=41) were compared with healthy subjects (n=25) and patients with cirrhosis (n=22) or acute liver failure (n=30). CD14+CD15-CD11b+HLA-DR- cells were identified as per definition of M-MDSC and detailed immunophenotypic analyses were performed. Suppression of T cell activation was assessed by mixed lymphocyte reaction. Assessment of innate immune function included cytokine expression in response to Toll-like receptor (TLR-2, TLR-4 and TLR-9) stimulation and phagocytosis assays using flow cytometry and live cell imaging-based techniques. RESULTS: Circulating CD14+CD15-CD11b+HLA-DR- M-MDSCs were markedly expanded in patients with ACLF (55% of CD14+ cells). M-MDSC displayed immunosuppressive properties, significantly decreasing T cell proliferation (p=0.01), producing less tumour necrosis factor-alpha/interleukin-6 in response to TLR stimulation (all p

Published

2018

5. Efficacy of rintatolimod in the treatment of chronic fatigue syndrome/myalgic encephalomyelitis (CFS/ME)

Author

William M. Mitchell

Subjects

0301 basic medicine, Agonist, Poly U, Rintatolimod, medicine.drug_class, Encephalomyelitis, dsRNA, clinical safety, Article, 03 medical and health sciences, clinical efficacy, Drug Profile, Interferon, medicine, Chronic fatigue syndrome, Animals, Humans, Pharmacology (medical), General Pharmacology, Toxicology and Pharmaceutics, RNA, Double-Stranded, Randomized Controlled Trials as Topic, clinical trials, Fatigue Syndrome, Chronic, business.industry, chronic fatigue/myalgic encephalomyelitis, General Medicine, medicine.disease, Protein kinase R, Immunity, Innate, 3. Good health, Toll-Like Receptor 3, Clinical trial, 030104 developmental biology, Poly I-C, TLR3, Immunology, TLR3 agonist, business, Ampligen, primate/non-primate disassociation of toxicity, medicine.drug

Abstract

Chronic fatigue syndrome/ Myalgic encephalomyelitis (CFS/ME) is a poorly understood seriously debilitating disorder in which disabling fatigue is an universal symptom in combination with a variety of variable symptoms. The only drug in advanced clinical development is rintatolimod, a mismatched double stranded polymer of RNA (dsRNA). Rintatolimod is a restricted Toll-Like Receptor 3 (TLR3) agonist lacking activation of other primary cellular inducers of innate immunity (e.g.- cytosolic helicases). Rintatolimod also activates interferon induced proteins that require dsRNA for activity (e.g.- 2ʹ-5ʹ adenylate synthetase, protein kinase R). Rintatolimod has achieved statistically significant improvements in primary endpoints in Phase II and Phase III double-blind, randomized, placebo-controlled clinical trials with a generally well tolerated safety profile and supported by open-label trials in the United States and Europe. The chemistry, mechanism of action, clinical trial data, and current regulatory status of rintatolimod for CFS/ME including current evidence for etiology of the syndrome are reviewed.

Published

2016