Qiu Yi-Ling, Gong Jing-Yu, Feng Jia-Yan, Wang Ren-Xue, Han Jun, Liu Teng, Lu Yi, Li Li-Ting, Zhang Mei-Hong, Sheps Jonathan A, Wang Neng-Li, Yan Yan-Yan, Li Jia-Qi, Chen Lian, Borchers Christoph H, Sipos Bence, Knisely A S, Ling Victor, Xing Qing-He, Wang Jian-She
The Center for Pediatric Liver Diseases, Children's Hospital of Fudan University, Shanghai, China.
Department of Pediatrics, Jinshan Hospital of Fudan University, Shanghai, China.
Hepatology. 2017 May;65(5):1655-1669. doi: 10.1002/hep.29020. Epub 2017 Mar 23.
Hereditary cholestasis in childhood and infancy with normal serum gamma-glutamyltransferase (GGT) activity is linked to several genes. Many patients, however, remain genetically undiagnosed. Defects in myosin VB (MYO5B; encoded by MYO5B) cause microvillus inclusion disease (MVID; MIM251850) with recurrent watery diarrhea. Cholestasis, reported as an atypical presentation in MVID, has been considered a side effect of parenteral alimentation. Here, however, we report on 10 patients who experienced cholestasis associated with biallelic, or suspected biallelic, mutations in MYO5B and who had neither recurrent diarrhea nor received parenteral alimentation. Seven of them are from two study cohorts, together comprising 31 undiagnosed low-GGT cholestasis patients; 3 are sporadic. Cholestasis in 2 patients was progressive, in 3 recurrent, in 2 transient, and in 3 uncategorized because of insufficient follow-up. Liver biopsy specimens revealed giant-cell change of hepatocytes and intralobular cholestasis with abnormal distribution of bile salt export pump (BSEP) at canaliculi, as well as coarse granular dislocation of MYO5B. Mass spectrometry of plasma demonstrated increased total bile acids, primary bile acids, and conjugated bile acids, with decreased free bile acids, similar to changes in BSEP-deficient patients. Literature review revealed that patients with biallelic mutations predicted to eliminate MYO5B expression were more frequent in typical MVID than in isolated-cholestasis patients (11 of 38 vs. 0 of 13).
MYO5B deficiency may underlie 20% of previously undiagnosed low-GGT cholestasis. MYO5B deficiency appears to impair targeting of BSEP to the canalicular membrane with hampered bile acid excretion, resulting in a spectrum of cholestasis without diarrhea. (Hepatology 2017;65:1655-1669).
儿童期和婴儿期血清γ-谷氨酰转移酶(GGT)活性正常的遗传性胆汁淤积与多个基因相关。然而,许多患者仍未得到基因诊断。肌球蛋白VB(MYO5B;由MYO5B编码)缺陷会导致微绒毛包涵体病(MVID;MIM251850)并伴有反复水样腹泻。胆汁淤积在MVID中被报道为非典型表现,一直被认为是肠外营养的副作用。然而,在此我们报告了10例因MYO5B双等位基因或疑似双等位基因突变而出现胆汁淤积的患者,他们既没有反复腹泻,也未接受过肠外营养。其中7例来自两个研究队列,这两个队列共有31例未确诊的低GGT胆汁淤积患者;3例为散发病例。2例患者的胆汁淤积呈进行性,3例呈复发性,2例呈短暂性,3例因随访不足而未分类。肝活检标本显示肝细胞巨细胞改变、小叶内胆汁淤积,胆小管处胆盐输出泵(BSEP)分布异常,以及MYO5B粗颗粒错位。血浆质谱分析显示总胆汁酸、初级胆汁酸和结合胆汁酸增加,游离胆汁酸减少,这与BSEP缺陷患者的变化相似。文献综述显示,预测会消除MYO5B表达的双等位基因突变患者在典型MVID中比孤立性胆汁淤积患者更常见(38例中有11例 vs. 13例中有0例)。
MYO5B缺陷可能是20%既往未确诊的低GGT胆汁淤积的病因。MYO5B缺陷似乎会损害BSEP靶向胆小管膜,阻碍胆汁酸排泄,导致一系列无腹泻的胆汁淤积。(《肝脏病学》2017年;65:1655 - 1669)
