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The endocannabinoid system in advanced liver cirrhosis: Pathophysiological implication and future perspectives

机译:晚期肝硬化中的大麻素系统:病理生理学意义和未来展望

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摘要

Endogenous cannabinoids (EC) are ubiquitous lipid signalling molecules providing different central and peripheral effects that are mediated mostly by the specific receptors CB1 and CB2. The EC system is highly upregulated during chronic liver disease and consistent experimental and clinical findings indicate that it plays a role in the pathogenesis of liver fibrosis and fatty liver disease associated with obesity, alcohol abuse and hepatitis C. Furthermore, a considerable number of studies have shown that EC and their receptors contribute to the pathogenesis of the cardio-circulatory disturbances occurring in advanced cirrhosis, such as portal hypertension, hyperdynamic circulatory syndrome and cirrhotic cardiomyopathy. More recently, the EC system has been implicated in the development of ascites, hepatic encephalopathy and the inflammatory response related to bacterial infection. Rimonabant, a selective CB1 antagonist, was the first drug acting on the EC system approved for the treatment of obesity. Unfortunately, it has been withdrawn from the market because of its neuropsychiatric side effects. Compounds able to target selectively the peripheral CB1 receptors are under evaluation. In addition, molecules stimulating CB2 receptor or modulating the activity of enzymes implicated in EC metabolism are promising areas of pharmacological research. Liver cirrhosis and the related complications represent an important target for the clinical application of these compounds.
机译:内源性大麻素(EC)是普遍存在的脂质信号分子,提供主要由特定受体CB1和CB2介导的不同的中枢和外周效应。 EC系统在慢性肝病期间高度上调,并且一致的实验和临床发现表明,它在与肥胖症,酗酒和丙型肝炎有关的肝纤维化和脂肪肝疾病的发病机理中起作用。此外,许多研究已经开展。研究表明,EC及其受体有助于晚期肝硬化发生的心血管循环障碍的发病机理,例如门脉高压,高动力循环综合征和肝硬化性心肌病。最近,EC系统与腹水,肝性脑病以及与细菌感染有关的炎症反应有关。利莫那班是一种选择性的CB1拮抗剂,是第一种被批准用于治疗肥胖症的作用于EC系统的药物。不幸的是,由于其神经精神方面的副作用,它已退出市场。能够选择性靶向外周CB1受体的化合物正在评估中。此外,刺激CB2受体或调节EC代谢中涉及的酶活性的分子是药理学研究中很有希望的领域。肝硬化和相关并发症是这些化合物临床应用的重要目标。

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