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Intermediate filament cytoskeleton of the liver in health and disease

机译:健康和疾病中肝脏的中间细丝细胞骨架

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摘要

Intermediate filaments (IFs) represent the largest cytoskeletal gene family comprising ~70 genes expressed in tissue specific manner. In addition to scaffolding function, they form complex signaling platforms and interact with various kinases, adaptor, and apoptotic proteins. IFs are established cytoprotectants and IF variants are associated with >30 human diseases. Furthermore, IF-containing inclusion bodies are characteristic features of several neurodegenerative, muscular, and other disorders. Acidic (type I) and basic keratins (type II) build obligatory type I and type II heteropolymers and are expressed in epithelial cells. Adult hepatocytes contain K8 and K18 as their only cytoplasmic IF pair, whereas cholangiocytes express K7 and K19 in addition. K8/K18-deficient animals exhibit a marked susceptibility to various toxic agents and Fas-induced apoptosis. In humans, K8/K18 variants predispose to development of end-stage liver disease and acute liver failure (ALF). K8/K18 variants also associate with development of liver fibrosis in patients with chronic hepatitis C. Mallory-Denk bodies (MDBs) are protein aggregates consisting of ubiquitinated K8/K18, chaperones and sequestosome1/p62 (p62) as their major constituents. MDBs are found in various liver diseases including alcoholic and non-alcoholic steatohepatitis and can be formed in mice by feeding hepatotoxic substances griseofulvin and 3,5-diethoxycarbonyl-1,4-dihydrocollidine (DDC). MDBs also arise in cell culture after transfection with K8/K18, ubiquitin, and p62. Major factors that determine MDB formation in vivo are the type of stress (with oxidative stress as a major player), the extent of stress-induced protein misfolding and resulting chaperone, proteasome and autophagy overload, keratin 8 excess, transglutaminase activation with transamidation of keratin 8 and p62 upregulation.
机译:中间丝(IF)代表最大的细胞骨架基因家族,包括以组织特异性方式表达的约70个基因。除脚手架功能外,它们还形成复杂的信号平台,并与各种激酶,衔接子和凋亡蛋白相互作用。 IF已确立为细胞保护剂,而IF变体与> 30种人类疾病相关。此外,含IF的包涵体是几种神经变性,肌肉和其他疾病的特征。酸性(I型)和碱性角蛋白(II型)可形成必不可少的I型和II型杂聚物,并在上皮细胞中表达。成年肝细胞含有K8和K18作为其唯一的细胞质IF对,而胆管细胞还表达K7和K19。 K8 / K18缺陷动物表现出对各种毒性剂和Fas诱导的细胞凋亡的明显易感性。在人类中,K8 / K18变体易患晚期肝病和急性肝衰竭(ALF)。 K8 / K18变体还与慢性丙型肝炎患者肝纤维化的发展有关。Mallory-Denk体(MDB)是由泛素化的K8 / K18,分子伴侣和sequestosome1 / p62(p62)作为其主要成分的蛋白质聚集体。 MDB存在于各种肝脏疾病中,包括酒精性和非酒精性脂肪性肝炎,可以通过喂食肝毒性物质灰黄霉素和3,5-二乙氧基羰基-1,4-二氢可力丁(DDC)在小鼠中形成。在用K8 / K18,泛素和p62转染后,细胞培养物中也会产生MDB。决定体内MDB形成的主要因素是应激的类型(氧化应激为主要因素),应激诱导的蛋白质错误折叠和由此产生的伴侣蛋白,蛋白酶体和自噬超负荷,角蛋白8过量,转谷氨酰胺酶活化以及角蛋白酰胺化的程度。 8和p62上调。

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