Synthetic glycolipid-based TLR4 antagonists negatively regulate TRIF-dependent TLR4 signalling in human macrophages.

IF 2.8 4区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Innate Immunity Pub Date : 2021-04-01 DOI:10.1177/17534259211005840
Charys Palmer, Fabio A Facchini, Richard Po Jones, Frank Neumann, Francesco Peri, Grisha Pirianov
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引用次数: 3

Abstract

TLRs, including TLR4, play a crucial role in inflammatory-based diseases, and TLR4 has been identified as a therapeutic target for pharmacological intervention. In previous studies, we investigated the potential of FP7, a novel synthetic glycolipid active as a TLR4 antagonist, to inhibit haematopoietic and non-haematopoietic MyD88-dependent TLR4 pro-inflammatory signalling. The main aim of this study was to investigate the action of FP7 and its derivative FP12 on MyD88-independent TLR4 signalling in THP-1 derived macrophages. Western blotting, Ab array and ELISA approaches were used to explore the effect of FP7 and FP12 on TRIF-dependent TLR4 functional activity in response to LPS and other endogenous TLR4 ligands in THP-1 macrophages. A different kinetic in the inhibition of endotoxin-driven TBK1, IRF3 and STAT1 phosphorylation was observed using different LPS chemotypes. Following activation of TLR4 by LPS, data revealed that FP7 and FP12 inhibited TBK1, IRF3 and STAT1 phosphorylation which was associated with down-regulation IFN-β and IP-10. Specific blockage of the IFN type one receptor showed that these novel molecules inhibited TRIF-dependent TLR4 signalling via IFN-β pathways. These results add novel information on the mechanism of action of monosaccharide FP derivatives. The inhibition of the TRIF-dependent pathway in human macrophages suggests potential therapeutic uses for these novel TLR4 antagonists in pharmacological interventions on inflammatory diseases.

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合成糖脂基TLR4拮抗剂负向调节人巨噬细胞中trf依赖的TLR4信号传导。
包括TLR4在内的tlr在炎症性疾病中起着至关重要的作用,TLR4已被确定为药物干预的治疗靶点。在之前的研究中,我们研究了FP7(一种新型合成糖脂,可作为TLR4拮抗剂)抑制造血和非造血myd88依赖性TLR4促炎信号的潜力。本研究的主要目的是研究FP7及其衍生物FP12对THP-1衍生巨噬细胞中myd88非依赖性TLR4信号传导的作用。采用Western blotting、Ab阵列和ELISA方法,探讨了FP7和FP12对THP-1巨噬细胞中trf依赖性TLR4功能活性响应LPS和其他内源性TLR4配体的影响。不同的LPS化学型对内毒素驱动的TBK1、IRF3和STAT1磷酸化的抑制动力学不同。LPS激活TLR4后,数据显示FP7和FP12抑制TBK1、IRF3和STAT1磷酸化,并下调IFN-β和IP-10。特异性阻断IFN 1型受体表明,这些新分子通过IFN-β途径抑制trf依赖性TLR4信号传导。这些结果为单糖FP衍生物的作用机制提供了新的信息。人类巨噬细胞中trf依赖通路的抑制表明,这些新型TLR4拮抗剂在炎症性疾病的药物干预中具有潜在的治疗用途。
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来源期刊
Innate Immunity
Innate Immunity 生物-免疫学
CiteScore
7.20
自引率
0.00%
发文量
20
审稿时长
6-12 weeks
期刊介绍: Innate Immunity is a highly ranked, peer-reviewed scholarly journal and is the official journal of the International Endotoxin & Innate Immunity Society (IEIIS). The journal welcomes manuscripts from researchers actively working on all aspects of innate immunity including biologically active bacterial, viral, fungal, parasitic, and plant components, as well as relevant cells, their receptors, signaling pathways, and induced mediators. The aim of the Journal is to provide a single, interdisciplinary forum for the dissemination of new information on innate immunity in humans, animals, and plants to researchers. The Journal creates a vehicle for the publication of articles encompassing all areas of research, basic, applied, and clinical. The subject areas of interest include, but are not limited to, research in biochemistry, biophysics, cell biology, chemistry, clinical medicine, immunology, infectious disease, microbiology, molecular biology, and pharmacology.
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