Daugherty C C, Setchell K D, Heubi J E, Balistreri W F
Department of Pathology, University of Cincinnati School of Medicine, Ohio.
Hepatology. 1993 Nov;18(5):1096-101.
Identical male twins and their brother, cholestatic from birth, with delta 4-3-oxosteroid 5 beta-reductase deficiency, were studied by serial liver biopsy. Spectrometry documented defective primary bile acid synthesis and markedly increased levels of atypical oxo and allo bile acids in urine and serum. Hepatocellular cholestasis and giant-cell transformation resolved in parallel with clinical and biochemical recovery during oral bile acid administration. In the twins, portal fibrosis stabilized at a mild level; they are well as 5-yr-olds at this writing. Follow-up biopsy in their brother at 8 mo was normal, and he is doing well at 3 yr of age. Hepatic ultrastructural alterations in all three were characterized by abnormalities of bile canaliculi including small bile plugs, diverticulae and latticelike elaborations of hepatocellular membranes adjacent to bile canaliculi that were shown to have resolved completely on subsequent biopsies. Eight additional cases have been detected on urine screening; only two of these patients have survived, on bile acid therapy. Early diagnosis and treatment improves the prognosis of this otherwise lethal inborn error of bile acid synthesis.
对一对同卵男性双胞胎及其弟弟进行了研究,他们自出生起就患有胆汁淤积症,患有δ4-3-氧代类固醇5β-还原酶缺乏症,通过连续肝脏活检进行观察。光谱分析记录了原发性胆汁酸合成缺陷,以及尿液和血清中非典型氧代和别胆酸水平显著升高。在口服胆汁酸治疗期间,肝细胞胆汁淤积和巨细胞转化与临床和生化指标的恢复同步缓解。在这对双胞胎中,门脉纤维化稳定在轻度水平;撰写本文时,他们5岁,情况良好。他们弟弟在8个月时的随访活检结果正常,3岁时情况良好。三人的肝脏超微结构改变均表现为胆小管异常,包括小胆栓、憩室以及胆小管附近肝细胞膜的网格状增生,后续活检显示这些异常已完全消失。通过尿液筛查又发现了另外8例病例;这些患者中只有2例在接受胆汁酸治疗后存活。早期诊断和治疗可改善这种原本致命的胆汁酸合成先天性缺陷的预后。
