Tornai David, Furi Istvan, Shen Zu T, Sigalov Alexander B, Coban Sahin, Szabo Gyongyi
Department of Medicine University of Massachusetts Medical School Worcester MA.
SignaBlok, Inc. Shrewsbury MA.
Hepatol Commun. 2018 Oct 29;3(1):99-115. doi: 10.1002/hep4.1269. eCollection 2019 Jan.
Alcoholic liver disease (ALD) is characterized by macrophage and neutrophil leukocyte recruitment and activation in the liver. Damage- and pathogen-associated molecular patterns contribute to a self-perpetuating proinflammatory state in ALD. Triggering receptor expressed on myeloid cells 1 (TREM-1) is a surface receptor that amplifies inflammation induced by toll-like receptors (TLRs) and is expressed on neutrophils and monocytes/macrophages. We hypothesized that TREM-1 signaling contributes to proinflammatory pathway activation in ALD. Using an ALD model in mice, we tested the effects of ligand-independent TREM-1 inhibitory peptides that were formulated into human high-density lipoprotein (HDL)-mimicking complexes GF9-HDL and GA/E31-HDL. As revealed , macrophages endocytosed these rationally designed complexes through scavenger receptors. A 5-week alcohol feeding with the Lieber-DeCarli diet in mice resulted in increased serum alanine aminotransferase (ALT), liver steatosis, and increased proinflammatory cytokines in the liver. TREM-1 messenger RNA (mRNA) expression was significantly increased in alcohol-fed mice, and TREM-1 inhibitors significantly reduced this increase. TREM-1 inhibition significantly attenuated alcohol-induced spleen tyrosine kinase (SYK) activation, an early event in both TLR4 and TREM-1 signaling. The TREM-1 inhibitors significantly inhibited macrophage (epidermal growth factor-like module-containing mucin-like hormone receptor-like 1 [F4/80], clusters of differentiation [CD]68) and neutrophil (lymphocyte antigen 6 complex, locus G [Ly6G] and myeloperoxidase [MPO]) markers and proinflammatory cytokines (monocyte chemoattractant protein 1 [MCP-1], tumor necrosis factor α [TNF-α], interleukin-1β [IL-1β], macrophage inflammatory protein 1α [MIP-1α]) at the mRNA level compared to the HDL vehicle. Administration of TREM-1 inhibitors ameliorated liver steatosis and early fibrosis markers (α-smooth muscle actin [αSMA] and procollagen1α [Pro-Col1α]) at the mRNA level in alcohol-fed mice. However, the HDL vehicle also reduced serum ALT and some cytokine protein levels in alcohol-fed mice, indicating HDL-related effects. HDL-delivered novel TREM-1 peptide inhibitors ameliorate early phases of inflammation and neutrophil and macrophage recruitment and activation in the liver and attenuate hepatocyte damage and liver steatosis. TREM-1 inhibition represents a promising therapeutic approach for further investigations in ALD.
酒精性肝病(ALD)的特征是肝脏中巨噬细胞和中性粒细胞的募集与活化。损伤相关分子模式和病原体相关分子模式会导致ALD中出现持续的促炎状态。髓系细胞触发受体1(TREM-1)是一种表面受体,可放大由Toll样受体(TLR)诱导的炎症,在中性粒细胞和单核细胞/巨噬细胞上表达。我们推测TREM-1信号传导有助于ALD中促炎途径的激活。利用小鼠ALD模型,我们测试了配体非依赖性TREM-1抑制肽的作用,这些肽被配制成人高密度脂蛋白(HDL)模拟复合物GF9-HDL和GA/E31-HDL。结果显示,巨噬细胞通过清道夫受体对这些合理设计的复合物进行内吞作用。给小鼠喂食5周的Lieber-DeCarli饮食会导致血清丙氨酸氨基转移酶(ALT)升高、肝脏脂肪变性以及肝脏中促炎细胞因子增加。在喂食酒精的小鼠中,TREM-1信使核糖核酸(mRNA)表达显著增加,而TREM-1抑制剂可显著降低这种增加。TREM-1抑制可显著减弱酒精诱导的脾酪氨酸激酶(SYK)活化,这是TLR4和TREM-1信号传导中的早期事件。与HDL载体相比,TREM-1抑制剂在mRNA水平上显著抑制巨噬细胞(含表皮生长因子样模块的黏蛋白样激素受体样1 [F4/80]、分化簇[CD]68)和中性粒细胞(淋巴细胞抗原6复合体,G位点[Ly6G]和髓过氧化物酶[MPO])标志物以及促炎细胞因子(单核细胞趋化蛋白1 [MCP-1]、肿瘤坏死因子α [TNF-α]、白细胞介素-1β [IL-1β]、巨噬细胞炎性蛋白1α [MIP-1α])。在喂食酒精的小鼠中,给予TREM-1抑制剂可在mRNA水平上改善肝脏脂肪变性和早期纤维化标志物(α-平滑肌肌动蛋白[αSMA]和前胶原1α [Pro-Col1α])。然而,HDL载体也降低了喂食酒精小鼠的血清ALT和一些细胞因子蛋白水平,表明存在HDL相关效应。HDL递送的新型TREM-1肽抑制剂可改善肝脏炎症的早期阶段以及中性粒细胞和巨噬细胞的募集与活化,并减轻肝细胞损伤和肝脏脂肪变性。TREM-1抑制代表了一种有前景的治疗方法,有待在ALD中进行进一步研究。
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