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酒精性和非酒精性脂肪性肝病:聚焦神经酰胺

Alcoholic and non-alcoholic fatty liver disease: Focus on ceramide.

作者信息

Nikolova-Karakashian Mariana

机构信息

Department of Physiology, University of Kentucky College of Medicine, 800 Rose Str., MS 508, Lexington, KY, 40536, United States.

出版信息

Adv Biol Regul. 2018 Dec;70:40-50. doi: 10.1016/j.jbior.2018.11.004. Epub 2018 Nov 14.

Abstract

Sphingolipids are class of metabolically distinct lipids that play structural and signaling functions in all organisms. Sphingolipid metabolism is deregulated during various diseases such as cancer, neurological and immune disorders, and metabolic syndrome. With the advancement of sphingo-lipidomics and sphingo-genomics, an understanding of the specific roles of ceramide, the quintessential bioactive sphingolipid, in fatty liver disease has taken shape. Two major pathways for ceramide generation, the de novo pathway and the sphingomyelinase pathway are activated in the course of both, the non-alcoholic and the alcoholic, forms of fatty liver disease. The mechanisms of activation of these two pathways are distinct and reflect the different disease etiology in each case; at the same time, common processes impacted by the resulting ceramide overproduction involve lipotoxocity, ER/mitochondrial stress, inflammation, and de-regulation of hepatic lipid metabolism. Studies in human patients and animal models have delineated specific enzymes and ceramide species that are involved at the different stages of the disease, and represent novel pharmaceutical targets for successful management of fatty liver disease.

摘要

鞘脂是一类代谢上不同的脂质,在所有生物体中发挥结构和信号传导功能。在各种疾病如癌症、神经和免疫紊乱以及代谢综合征期间,鞘脂代谢失调。随着鞘脂组学和鞘脂基因组学的发展,对神经酰胺(典型的生物活性鞘脂)在脂肪肝疾病中的具体作用的理解已具雏形。神经酰胺生成的两条主要途径,即从头合成途径和鞘磷脂酶途径,在非酒精性和酒精性两种形式的脂肪肝疾病过程中均被激活。这两条途径的激活机制不同,反映了每种情况下不同的疾病病因;同时,由神经酰胺过量产生所影响的共同过程包括脂毒性、内质网/线粒体应激、炎症以及肝脏脂质代谢失调。对人类患者和动物模型的研究已经明确了在疾病不同阶段涉及的特定酶和神经酰胺种类,它们代表了成功治疗脂肪肝疾病的新型药物靶点。

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