Notch信号通路的阻断会促进对乙酰氨基酚诱导的肝损伤。
Blockade of Notch signaling promotes acetaminophen-induced liver injury.
作者信息
Jiang Longfeng, Ke Michael, Yue Shi, Xiao Wen, Yan Youde, Deng Xiaozhao, Ying Qi-Long, Li Jun, Ke Bibo
机构信息
Department of Infectious Diseases, the First Affiliated Hospital, Nanjing Medical University, Nanjing, China.
The Dumont-UCLA Transplant Center, Department of Surgery, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA.
出版信息
Immunol Res. 2017 Jun;65(3):739-749. doi: 10.1007/s12026-017-8913-3.
Liver injury after experimental acetaminophen treatment is mediated both by direct hepatocyte injury through a P450-generated toxic metabolite and indirectly by activated liver Kupffer cells and neutrophils. This study was designed to investigate the role of Notch signaling in the regulation of innate immune responses in acetaminophen (APAP)-induced liver injury. Using a mouse model of APAP-induced liver injury, wild-type (WT) and toll-like receptor 4 knockout (TLR4 KO) mice were injected intraperitoneally with APAP or PBS. Some animals were injected with γ-secretase inhibitor DAPT or DMSO vehicle. For the in vitro study, bone marrow-derived macrophages (BMMs) were transfected with Notch1 siRNA, TLR4 siRNA, and non-specific (NS) siRNA and stimulated with LPS. Indeed, paracetamol/acetaminophen-induced liver damage was worse after Notch blockade with DAPT in wild-type mice, which was accompanied by significantly increased ALT levels, diminished hairy and enhancer of split-1 (Hes1), and phosphorylated Stat3 and Akt but enhanced high mobility group box 1 (HMGB1), TLR4, NF-κB, and NLRP3 activation after APAP challenge. Mice receiving DAPT increased macrophage and neutrophil accumulation and hepatocellular apoptosis. However, TLR4 KO mice that received DAPT reduced APAP-induced liver damage and NF-κB, NLRP3, and cleaved caspase-1 activation. BMMs transfected with Notch1 siRNA reduced Hes1 and phosphorylated Stat3 and Akt but augmented HMGB1, TLR4, NF-κB, and NLRP3. Furthermore, TLR4 siRNA knockdown resulted in decreased NF-κB and NLRP3 and cleaved caspase-1 and IL-1β levels following LPS stimulation. These results demonstrate that Notch signaling regulates innate NLRP3 inflammasome activation through regulation of HMGB1/TLR4/NF-κB activation in APAP-induced liver injury. Our novel findings underscore the critical role of the Notch1-Hes1 signaling cascade in the regulation of innate immunity in APAP-triggered liver inflammation. This might imply a novel therapeutic potential for the drug-induced damage-associated lethal hepatitis.
实验性对乙酰氨基酚治疗后的肝损伤,既由细胞色素P450生成的毒性代谢产物直接导致肝细胞损伤介导,也由活化的肝库普弗细胞和中性粒细胞间接介导。本研究旨在探讨Notch信号在对乙酰氨基酚(APAP)诱导的肝损伤中对先天免疫反应调节的作用。使用APAP诱导的肝损伤小鼠模型,野生型(WT)和Toll样受体4基因敲除(TLR4 KO)小鼠腹腔注射APAP或PBS。部分动物注射γ-分泌酶抑制剂DAPT或二甲基亚砜(DMSO)溶剂。对于体外研究,用Notch1小干扰RNA(siRNA)、TLR4 siRNA和非特异性(NS)siRNA转染骨髓来源的巨噬细胞(BMMs),并用脂多糖(LPS)刺激。的确,在野生型小鼠中用DAPT阻断Notch后,对乙酰氨基酚/扑热息痛诱导的肝损伤更严重,伴有谷丙转氨酶(ALT)水平显著升高、毛状分裂增强子1(Hes1)减少、磷酸化信号转导和转录激活因子3(Stat3)及蛋白激酶B(Akt)减少,但在APAP攻击后高迁移率族蛋白B1(HMGB1)、TLR4、核因子κB(NF-κB)和NLR家族含pyrin结构域蛋白3(NLRP3)激活增强。接受DAPT的小鼠巨噬细胞和中性粒细胞积聚增加,肝细胞凋亡增加。然而,接受DAPT的TLR4 KO小鼠减轻了APAP诱导的肝损伤以及NF-κB、NLRP3和裂解的半胱天冬酶-1激活。用Notch1 siRNA转染的BMMs减少了Hes1以及磷酸化Stat3和Akt,但增加了HMGB1、TLR4、NF-κB和NLRP3。此外,TLR4 siRNA敲低导致LPS刺激后NF-κB和NLRP3以及裂解的半胱天冬酶-1和白细胞介素-1β水平降低。这些结果表明,在APAP诱导的肝损伤中,Notch信号通过调节HMGB1/TLR4/NF-κB激活来调节先天NLRP3炎性小体激活。我们的新发现强调了Notch1-Hes1信号级联在APAP触发的肝脏炎症先天免疫调节中的关键作用。这可能意味着对药物诱导的损伤相关性致死性肝炎具有新的治疗潜力。
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