白细胞介素-1受体样蛋白1通过限制肝巨噬细胞中核因子κB的激活来预防酒精性肝损伤。
IL-1 receptor like 1 protects against alcoholic liver injury by limiting NF-κB activation in hepatic macrophages.
作者信息
Wang Meng, Shen Guannan, Xu Liangguo, Liu Xiaodong, Brown Jared M, Feng Dechun, Ross Ruth Ann, Gao Bin, Liangpunsakul Suthat, Ju Cynthia
机构信息
Skaggs School of Pharmacy and Pharmaceutical Sciences, University of Colorado Anschutz Medical Campus, USA.
School of Life Science, Jiangxi Normal University, China.
出版信息
J Hepatol. 2017 Sep 21. doi: 10.1016/j.jhep.2017.08.023.
BACKGROUND & AIM: Alcohol consumption increases intestinal permeability and causes damage to hepatocytes, leading to the release of pathogen- and damage-associated molecular pattern molecules (PAMPs and DAMPs), stimulating hepatic macrophages and activating NF-κB. The resultant inflammation exacerbates alcoholic liver disease (ALD). However, much less is known about the mechanisms attenuating inflammation and preventing disease progression in most heavy drinkers. Interleukin (IL)-33 is a DAMP (alarmin) released from dead cells that acts through its receptor, IL-1 receptor like 1 (ST2). ST2 signaling has been reported to either stimulate or inhibit NF-κB activation. The role of IL-33/ST2 in ALD has not been studied.
METHODS
Serum levels of IL-33 and its decoy receptor, soluble ST2 (sST2) were measured in ALD patients. Alcohol-induced liver injury, inflammation and hepatic macrophage activation were compared between wild-type, IL-33 and ST2 mice in several models.
RESULTS
Elevation of serum IL-33 and sST2 were only observed in patients with severe decompensated ALD. Consistently, in mice with mild ALD without significant cell death and IL-33 release, IL-33 deletion did not affect alcohol-induced liver damage. However, ST2-deletion exacerbated ALD, through enhancing NF-κB activation in liver macrophages. In contrast, when extracellular IL-33 was markedly elevated, liver injury and inflammation were attenuated in both IL-33 and ST2 mice compared to wild-type mice.
CONCLUSION
Our data revealed a dichotomous role of IL-33/ST2 signaling during ALD development. At early and mild stages, ST2 restrains the inflammatory activation of hepatic macrophages, through inhibiting NF-κB, and plays a protective function in an IL-33-independent fashion. During severe liver injury, significant cell death and marked IL-33 release occur, which triggers IL-33/ST2 signaling and exacerbates tissue damage.
LAY SUMMARY
In mild ALD, ST2 negatively regulates the inflammatory activation of hepatic macrophages, thereby protecting against alcohol-induced liver damage, whereas in the case of severe liver injury, the release of extracellular IL-33 may exacerbate tissue inflammation by triggering the canonical IL-33/ST2L signaling in hepatic macrophages.
背景与目的
饮酒会增加肠道通透性并损害肝细胞,导致病原体相关分子模式分子和损伤相关分子模式分子(PAMPs和DAMPs)释放,刺激肝巨噬细胞并激活核因子κB(NF-κB)。由此产生的炎症会加重酒精性肝病(ALD)。然而,对于大多数重度饮酒者减轻炎症和预防疾病进展的机制,人们了解得还很少。白细胞介素(IL)-33是一种从死亡细胞释放的DAMP(警报素),通过其受体白细胞介素-1受体样1(ST2)发挥作用。据报道,ST2信号传导既能刺激也能抑制NF-κB激活。IL-33/ST2在ALD中的作用尚未得到研究。
方法
检测了ALD患者血清中IL-33及其诱饵受体可溶性ST2(sST2)的水平。在几种模型中,比较了野生型、IL-33基因敲除和ST2基因敲除小鼠的酒精性肝损伤、炎症和肝巨噬细胞激活情况。
结果
仅在严重失代偿性ALD患者中观察到血清IL-33和sST2升高。同样,在无明显细胞死亡和IL-33释放的轻度ALD小鼠中,IL-33基因敲除不影响酒精性肝损伤。然而,ST2基因敲除通过增强肝巨噬细胞中的NF-κB激活而加重了ALD。相反,当细胞外IL-33明显升高时,与野生型小鼠相比,IL-33基因敲除小鼠和ST2基因敲除小鼠的肝损伤和炎症均减轻。
结论
我们的数据揭示了IL-33/ST2信号传导在ALD发展过程中的双重作用。在早期和轻度阶段,ST2通过抑制NF-κB来抑制肝巨噬细胞的炎症激活,并以不依赖IL-33的方式发挥保护作用。在严重肝损伤期间,会发生明显的细胞死亡和显著的IL-33释放,这会触发IL-33/ST2信号传导并加剧组织损伤。
简要概述
在轻度ALD中,ST2负向调节肝巨噬细胞的炎症激活,从而预防酒精性肝损伤,而在严重肝损伤的情况下,细胞外IL-33的释放可能通过触发肝巨噬细胞中经典的IL-33/ST2L信号传导而加剧组织炎症。
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