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Hepatology. 2017 Feb;65(2):560-570. doi: 10.1002/hep.28929. Epub 2016 Dec 24.
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ABCB4、ABCB11 和 ATP8B1 变异患者成人发病肝病的临床表型。

Clinical phenotype of adult-onset liver disease in patients with variants in ABCB4, ABCB11, and ATP8B1.

机构信息

Institute of Liver StudiesKing's College HospitalLondonUK.

Institute of Liver Studies, Immunology & Microbial SciencesKing's College LondonLondonUK.

出版信息

Hepatol Commun. 2022 Oct;6(10):2654-2664. doi: 10.1002/hep4.2051. Epub 2022 Jul 27.

DOI:10.1002/hep4.2051
PMID:35894240
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9512461/
Abstract

Variants in ATP8B1, ABCB11, and ABCB4 underlie the most prevalent forms of progressive familial intrahepatic cholestasis. We aim to describe variants in these genes in a cohort of patients with adult-onset liver disease, and explore a genotype-phenotype correlation. Patients with onset of liver disease aged above 18 who underwent sequencing of cholestasis genes for clinical purposes over a 5-year period were identified. Bioinformatic analysis of variants was performed. Liver histology was evaluated in patients with variants. Of the 356 patients tested, at least one variant was identified in 101 (28.4%): 46 ABCB4, 35 ABCB11, and 28 ATP8B1. Patients with ABCB4 variants had chronic liver disease (71.7%) and pregnancy-associated liver dysfunction (75%), with a younger age of onset in more severe genotypes (p = 0.046). ABCB11 variants presented with pregnancy-associated liver dysfunction (82.4%) and acute/episodic cholestasis (40%), with no association between age of onset and genotype severity. ATP8B1 variants were associated with chronic liver disease (75%); however, they were commonly seen in patients with an alternate etiology of liver disease and variants were of low predicted pathogenicity. In adults with suspected genetic cholestasis, variants in cholestasis genes were frequently identified and were likely to contribute to the development of liver disease, particularly ABCB4 and ABCB11. Variants were often in heterozygous state, and they should no longer be considered recessive Mendelian traits. Sequencing cholestasis genes in selected patients with adult-onset disease should be considered, with interpretation in close collaboration with histopathologists and geneticists.

摘要

ATP8B1、ABCB11 和 ABCB4 中的变异是最常见的进行性家族性肝内胆汁淤积症的基础。我们旨在描述在一组患有成人发病肝病的患者中这些基因的变异,并探索基因型-表型相关性。通过对 5 年内因临床目的而接受胆汁淤积症基因测序的 18 岁以上发病的肝病患者进行鉴定,确定了患者。对变异进行了生物信息学分析。对有变异的患者进行了肝组织学评估。在 356 名接受测试的患者中,有 101 名(28.4%)至少发现了一个变异:46 个 ABCB4、35 个 ABCB11 和 28 个 ATP8B1。ABCB4 变异患者有慢性肝病(71.7%)和妊娠相关的肝功能障碍(75%),更严重基因型的发病年龄更早(p=0.046)。ABCB11 变异与妊娠相关的肝功能障碍(82.4%)和急性/间歇性胆汁淤积症(40%)有关,发病年龄与基因型严重程度之间无关联。ATP8B1 变异与慢性肝病有关(75%);然而,它们常见于有其他病因的肝病患者,变异的预测致病性较低。在怀疑有遗传性胆汁淤积症的成年人中,经常发现胆汁淤积症基因的变异,这些变异可能导致肝病的发生,特别是 ABCB4 和 ABCB11。变异通常为杂合状态,它们不再被认为是隐性孟德尔性状。应考虑对患有成人发病疾病的选定患者进行胆汁淤积症基因测序,并与组织病理学家和遗传学家密切合作进行解释。