Ku N O, Wright T L, Terrault N A, Gish R, Omary M B
Department of Medicine, VA Palo Alto Health Care System, California 94304, USA.
J Clin Invest. 1997 Jan 1;99(1):19-23. doi: 10.1172/JCI119127.
Mutations in 11 of the more than 20 keratin intermediate filaments cause several epidermal and oral associated diseases. No disease-associated mutations have been described in keratin 8 or 18 (K8/18) which are the major keratin pair in simple-type epithelia, as found in the liver, pancreas, and intestine. However, transgenic mice that express mutant keratin 18 develop chronic hepatitis, and have an increased susceptibility to drug-induced hepatotoxicity. Also, ectopic expression of epidermal K14 in mouse liver results in chronic hepatitis, and disruption of mouse K8 leads to embryo lethality with extensive liver hemorrhage. We tested if patients with liver disease of unknown cause may harbor mutations in K18. We describe a his127-->leu (H127L) K18 mutation in a patient with cryptogenic cirrhosis that is germline transmitted. The K18 H127L isolated from the liver explant, or after expression in bacteria, showed an altered migration on two-dimensional gel analysis as compared with normal human liver or bacterially expressed K18. Electron microscopy of in vitro assembled K18 H127L and wild type K8 showed an assembly defect as compared with normal K8/18 assembly. Our results suggest that mutations in K18 may be predispose to, or result in cryptogenic cirrhosis in humans.
20多种角蛋白中间丝中的11种发生突变会引发多种与表皮和口腔相关的疾病。在肝、胰腺和肠道等简单上皮组织中作为主要角蛋白对的角蛋白8或18(K8/18),尚未发现与疾病相关的突变。然而,表达突变型角蛋白18的转基因小鼠会发展为慢性肝炎,并且对药物诱导的肝毒性敏感性增加。此外,小鼠肝脏中表皮K14的异位表达会导致慢性肝炎,而小鼠K8的破坏会导致胚胎致死并伴有广泛的肝脏出血。我们测试了病因不明的肝病患者是否可能携带K18突变。我们描述了一名隐源性肝硬化患者中存在一种可通过种系传递的his127-->leu(H127L)K18突变。从肝脏外植体分离的或在细菌中表达后的K18 H127L,与正常人类肝脏或细菌表达的K18相比,在二维凝胶分析中显示出迁移改变。与正常K8/18组装相比,体外组装的K18 H127L和野生型K8的电子显微镜检查显示存在组装缺陷。我们的结果表明,K18突变可能使人易患或导致人类隐源性肝硬化。