TREM-2 在胆汁淤积中发挥保护作用,充当炎症的负调节剂。
TREM-2 plays a protective role in cholestasis by acting as a negative regulator of inflammation.
机构信息
Department of Liver and Gastrointestinal Diseases, Biodonostia Research Institute, Donostia University Hospital, University of the Basque Country (UPV-EHU), Donostia-San Sebastian, Spain.
Institute for Vascular Biology, Center for Physiology and Pharmacology, Medical University Vienna, Vienna, Austria; Christian Doppler Laboratory for Arginine Metabolism in Rheumatoid Arthritis and Multiple Sclerosis, Vienna, Austria.
出版信息
J Hepatol. 2022 Oct;77(4):991-1004. doi: 10.1016/j.jhep.2022.05.044. Epub 2022 Jun 22.
BACKGROUND & AIMS: Inflammation, particularly that mediated by bacterial components translocating from the gut to the liver and binding to toll-like receptors (TLRs), is central to cholestatic liver injury. The triggering receptor expressed on myeloid cells-2 (TREM-2) inhibits TLR-mediated signaling and exerts a protective role in hepatocellular injury and carcinogenesis. This study aims to evaluate the role of TREM-2 in cholestasis.
METHODS
TREM-2 expression was analyzed in the livers of patients with primary biliary cholangitis (PBC) or primary sclerosing cholangitis (PSC), and in mouse models of cholestasis. Wild-type (WT) and Trem-2 deficient (Trem-2) mice were subjected to experimental cholestasis and gut sterilization. Primary cultured Kupffer cells were incubated with lipopolysaccharide and/or ursodeoxycholic acid (UDCA) and inflammatory responses were analyzed.
RESULTS
TREM-2 expression was upregulated in the livers of patients with PBC or PSC, and in murine models of cholestasis. Compared to WT, the response to bile duct ligation (BDL)-induced obstructive cholestasis or alpha-naphtylisothiocyanate (ANIT)-induced cholestasis was exacerbated in Trem-2 mice. This was characterized by enhanced necroptotic cell death, inflammatory responses and biliary expansion. Antibiotic treatment partially abrogated the effects observed in Trem-2 mice after BDL. Experimental overexpression of TREM-2 in the liver of WT mice downregulated ANIT-induced IL-33 expression and neutrophil recruitment. UDCA regulated Trem-1 and Trem-2 expression in primary cultured mouse Kupffer cells and dampened inflammatory gene transcription via a TREM-2-dependent mechanism.
CONCLUSIONS
TREM-2 acts as a negative regulator of inflammation during cholestasis, representing a novel potential therapeutic target.
LAY SUMMARY
Cholestasis (the reduction or cessation of bile flow) causes liver injury. This injury is exacerbated when gut-derived bacterial components interact with receptors (specifically Toll-like receptors or TLRs) on liver-resident immune cells, promoting inflammation. Herein, we show that the anti-inflammatory receptor TREM-2 dampens TLR-mediated signaling and hence protects against cholestasis-induced liver injury. Thus, TREM-2 could be a potential therapeutic target in cholestasis.
背景与目的
炎症,尤其是由从肠道转移到肝脏并与 Toll 样受体(TLR)结合的细菌成分介导的炎症,是胆汁淤积性肝损伤的核心。髓样细胞表达的触发受体-2(TREM-2)抑制 TLR 介导的信号转导,并在肝细胞损伤和癌变中发挥保护作用。本研究旨在评估 TREM-2 在胆汁淤积中的作用。
方法
分析原发性胆汁性胆管炎(PBC)或原发性硬化性胆管炎(PSC)患者和胆汁淤积模型小鼠肝脏中 TREM-2 的表达。野生型(WT)和 Trem-2 缺陷(Trem-2)小鼠接受实验性胆汁淤积和肠道消毒。原代培养的枯否细胞与脂多糖和/或熊去氧胆酸(UDCA)孵育,并分析炎症反应。
结果
PBC 或 PSC 患者和胆汁淤积模型小鼠肝脏中 TREM-2 的表达上调。与 WT 相比,Trem-2 小鼠对胆管结扎(BDL)诱导的梗阻性胆汁淤积或α-萘异硫氰酸酯(ANIT)诱导的胆汁淤积的反应更为严重。其特征为坏死性细胞死亡、炎症反应和胆管扩张增强。抗生素治疗部分消除了 BDL 后 Trem-2 小鼠观察到的作用。WT 小鼠肝脏中 TREM-2 的实验过表达下调了 ANIT 诱导的 IL-33 表达和中性粒细胞募集。UDCA 调节原代培养的小鼠枯否细胞中 Trem-1 和 Trem-2 的表达,并通过 TREM-2 依赖的机制抑制炎症基因转录。
结论
TREM-2 在胆汁淤积时作为炎症的负调节剂发挥作用,代表了一个新的潜在治疗靶点。
概要
胆汁淤积(胆汁流动减少或停止)可导致肝脏损伤。当肠道来源的细菌成分与肝脏固有免疫细胞上的受体(特别是 Toll 样受体或 TLR)相互作用时,这种损伤会加剧,从而促进炎症。在此,我们表明抗炎受体 TREM-2 可抑制 TLR 介导的信号转导,从而防止胆汁淤积引起的肝损伤。因此,TREM-2 可能是胆汁淤积的潜在治疗靶点。
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