Peng Cheng, Stewart Alastair G, Woodman Owen L, Ritchie Rebecca H, Qin Cheng Xue
Drug Discovery Biology, Monash Institute of Pharmaceutical Sciences, Melbourne, VIC, Australia.
Baker Heart & Diabetes Institute, Melbourne, VIC, Australia.
Front Pharmacol. 2020 Dec 3;11:603926. doi: 10.3389/fphar.2020.603926. eCollection 2020.
Non-alcoholic steatohepatitis (NASH) develops from non-alcoholic fatty liver disease (NAFLD). Currently, around 25% of the population is estimated to have NAFLD, and 25% of NAFLD patients are estimated to have NASH. NASH is typically characterized by liver steatosis inflammation, and fibrosis driven by metabolic disruptions such as obesity, diabetes, and dyslipidemia. NASH patients with significant fibrosis have increased risk of developing cirrhosis and liver failure. Currently, NASH is the second leading cause for liver transplant in the United States. More importantly, the risk of developing hepatocellular carcinoma from NASH has also been highlighted in recent studies. Patients may have NAFLD for years before progressing into NASH. Although the pathogenesis of NASH is not completely understood, the current "multiple-hits" hypothesis suggests that in addition to fat accumulation, elevated oxidative and ER stress may also drive liver inflammation and fibrosis. The development of clinically relevant animal models and pharmacological treatments for NASH have been hampered by the limited understanding of the disease mechanism and a lack of sensitive, non-invasive diagnostic tools. Currently, most pre-clinical animal models are divided into three main groups which includes: genetic models, diet-induced, and toxin + diet-induced animal models. Although dietary models mimic the natural course of NASH in humans, the models often only induce mild liver injury. Many genetic and toxin + diet-induced models rapidly induce the development of metabolic disruption and serious liver injury, but not without their own shortcomings. This review provides an overview of the "multiple-hits" hypothesis and an evaluation of the currently existing animal models of NASH. This review also provides an update on the available interventions for managing NASH as well as pharmacological agents that are currently undergoing clinical trials for the treatment of NASH.
非酒精性脂肪性肝炎(NASH)由非酒精性脂肪性肝病(NAFLD)发展而来。目前,据估计约25%的人口患有NAFLD,且据估计25%的NAFLD患者患有NASH。NASH的典型特征是肝脂肪变性、炎症以及由肥胖、糖尿病和血脂异常等代谢紊乱驱动的纤维化。具有显著纤维化的NASH患者发生肝硬化和肝衰竭的风险增加。目前,NASH是美国肝移植的第二大主要原因。更重要的是,近期研究也强调了NASH患者发生肝细胞癌的风险。患者在进展为NASH之前可能已患有NAFLD数年。尽管NASH的发病机制尚未完全明确,但目前的“多重打击”假说表明,除脂肪堆积外,氧化应激和内质网应激升高也可能促使肝脏发生炎症和纤维化。对疾病机制的有限了解以及缺乏敏感的非侵入性诊断工具阻碍了NASH临床相关动物模型和药物治疗的发展。目前,大多数临床前动物模型主要分为三大类,包括:基因模型、饮食诱导模型和毒素+饮食诱导模型。尽管饮食模型模拟了人类NASH的自然病程,但这些模型往往仅诱导轻度肝损伤。许多基因模型和毒素+饮食诱导模型能迅速诱导代谢紊乱和严重肝损伤的发生,但也各有其不足之处。本综述概述了“多重打击”假说,并对目前现有的NASH动物模型进行了评估。本综述还介绍了用于管理NASH的现有干预措施以及目前正在进行NASH治疗临床试验的药物。
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