Departments of Pediatrics, National Taiwan University College of Medicine and Children's Hospital, 17F, No. 8, Chung Shan S. Rd, Taipei, 100, Taiwan.
Department of Medical Education and Bioethics, National Taiwan University College of Medicine, No. 1, Jen Ai Rd Section 1, Taipei, 100, Taiwan.
J Biomed Sci. 2018 Oct 26;25(1):75. doi: 10.1186/s12929-018-0475-8.
Jaundice is a common symptom of inherited or acquired liver diseases or a manifestation of diseases involving red blood cell metabolism. Recent progress has elucidated the molecular mechanisms of bile metabolism, hepatocellular transport, bile ductular development, intestinal bile salt reabsorption, and the regulation of bile acids homeostasis.
The major genetic diseases causing jaundice involve disturbances of bile flow. The insufficiency of bile salts in the intestines leads to fat malabsorption and fat-soluble vitamin deficiencies. Accumulation of excessive bile acids and aberrant metabolites results in hepatocellular injury and biliary cirrhosis. Progressive familial intrahepatic cholestasis (PFIC) is the prototype of genetic liver diseases manifesting jaundice in early childhood, progressive liver fibrosis/cirrhosis, and failure to thrive. The first three types of PFICs identified (PFIC1, PFIC2, and PFIC3) represent defects in FIC1 (ATP8B1), BSEP (ABCB11), or MDR3 (ABCB4). In the last 5 years, new genetic disorders, such as TJP2, FXR, and MYO5B defects, have been demonstrated to cause a similar PFIC phenotype. Inborn errors of bile acid metabolism also cause progressive cholestatic liver injuries. Prompt differential diagnosis is important because oral primary bile acid replacement may effectively reverse liver failure and restore liver functions. DCDC2 is a newly identified genetic disorder causing neonatal sclerosing cholangitis. Other cholestatic genetic disorders may have extra-hepatic manifestations, such as developmental disorders causing ductal plate malformation (Alagille syndrome, polycystic liver/kidney diseases), mitochondrial hepatopathy, and endocrine or chromosomal disorders. The diagnosis of genetic liver diseases has evolved from direct sequencing of a single gene to panel-based next generation sequencing. Whole exome sequencing and whole genome sequencing have been actively investigated in research and clinical studies. Current treatment modalities include medical treatment (ursodeoxycholic acid, cholic acid or chenodeoxycholic acid), surgery (partial biliary diversion and liver transplantation), symptomatic treatment for pruritus, and nutritional therapy. New drug development based on gene-specific treatments, such as apical sodium-dependent bile acid transporter (ASBT) inhibitor, for BSEP defects are underway.
Understanding the complex pathways of jaundice and cholestasis not only enhance insights into liver pathophysiology but also elucidate many causes of genetic liver diseases and promote the development of novel treatments.
黄疸是遗传性或获得性肝病的常见症状,也是涉及红细胞代谢疾病的表现。近年来,人们对胆汁代谢、肝细胞转运、胆管发育、肠道胆汁盐重吸收以及胆汁酸稳态调节的分子机制有了更深入的了解。
引起黄疸的主要遗传疾病涉及胆汁流动障碍。肠道内胆汁盐不足会导致脂肪吸收不良和脂溶性维生素缺乏。过量胆汁酸和异常代谢物的积累会导致肝细胞损伤和胆汁性肝硬化。进行性家族性肝内胆汁淤积症(PFIC)是一种遗传性肝病的原型,其特征是在幼儿期出现黄疸、进行性肝纤维化/肝硬化和生长不良。已确定的前三种 PFIC(PFIC1、PFIC2 和 PFIC3)代表 FIC1(ATP8B1)、BSEP(ABCB11)或 MDR3(ABCB4)的缺陷。在过去的 5 年中,已经证明新的遗传疾病,如 TJP2、FXR 和 MYO5B 缺陷,会导致类似的 PFIC 表型。胆汁酸代谢的先天性错误也会导致进行性胆汁淤积性肝损伤。及时进行鉴别诊断非常重要,因为口服初级胆汁酸替代治疗可能有效逆转肝衰竭并恢复肝功能。DCDC2 是一种新发现的导致新生儿硬化性胆管炎的遗传疾病。其他胆汁淤积性遗传疾病可能有肝外表现,如胆管板畸形(Alagille 综合征、多囊肝/肾病)、线粒体肝病、内分泌或染色体疾病。遗传肝病的诊断已经从单一基因的直接测序发展到基于面板的下一代测序。外显子组测序和全基因组测序已在研究和临床研究中得到积极探索。目前的治疗方法包括药物治疗(熊去氧胆酸、胆酸或鹅脱氧胆酸)、手术(部分胆道分流和肝移植)、瘙痒对症治疗和营养治疗。基于基因特异性治疗的新药开发,如针对 BSEP 缺陷的顶端钠依赖性胆汁酸转运体(ASBT)抑制剂,正在进行中。
了解黄疸和胆汁淤积的复杂途径不仅可以加深对肝脏病理生理学的理解,还可以阐明许多遗传肝病的病因,并促进新疗法的发展。
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