对一大群胆汁淤积症患者的 FIC1、BSEP 和 MDR3 进行测序,揭示了大量不同的遗传变异。
Sequencing of FIC1, BSEP and MDR3 in a large cohort of patients with cholestasis revealed a high number of different genetic variants.
机构信息
Department of Gastroenterology, Hepatology and Infectious Diseases, University Hospital Düsseldorf, Heinrich Heine University Düsseldorf, Germany.
Institute for Pharmaceutical and Medicinal Chemistry, Heinrich Heine University Düsseldorf, Germany.
出版信息
J Hepatol. 2017 Dec;67(6):1253-1264. doi: 10.1016/j.jhep.2017.07.004. Epub 2017 Jul 19.
BACKGROUND & AIMS: The bile salt export pump (BSEP, ABCB11), multidrug resistance protein 3 (MDR3, ABCB4) and the ATPase familial intrahepatic cholestasis 1 (FIC1, ATP8B1) mediate bile formation. This study aimed to determine the contribution of mutations and common variants in the FIC1, BSEP and MDR3 genes to cholestatic disorders of differing disease onset and severity.
METHODS
Coding exons with flanking intron regions of ATP8B1, ABCB11, and ABCB4 were sequenced in cholestatic patients with assumed genetic cause. The effects of new variants were evaluated by bioinformatic tools and 3D protein modeling.
RESULTS
In 427 patients with suspected inherited cholestasis, 149 patients carried at least one disease-causing mutation in FIC1, BSEP or MDR3, respectively. Overall, 154 different mutations were identified, of which 25 were novel. All 13 novel missense mutations were disease-causing according to bioinformatics analyses and homology modeling. Eighty-two percent of patients with at least one disease-causing mutation in either of the three genes were children. One or more common polymorphism(s) were found in FIC1 in 35.3%, BSEP in 64.3% and MDR3 in 72.6% of patients without disease-causing mutations in the respective gene. Minor allele frequencies of common polymorphisms in BSEP and MDR3 varied in our cohort compared to the general population, as described by gnomAD. However, differences in ethnic background may contribute to this effect.
CONCLUSIONS
In a large cohort of patients, 154 different variants were detected in FIC1, BSEP, and MDR3, 25 of which were novel. In our cohort, frequencies for risk alleles of BSEP (p.V444A) and MDR3 (p.I237I) polymorphisms were significantly overrepresented in patients without disease-causing mutation in the respective gene, indicating that these common variants can contribute to a cholestatic phenotype.
LAY SUMMARY
FIC1, BSEP, and MDR3 represent hepatobiliary transport proteins essential for bile formation. Genetic variants in these transporters underlie a broad spectrum of cholestatic liver diseases. To confirm a genetic contribution to the patients' phenotypes, gene sequencing of these three major cholestasis-related genes was performed in 427 patients and revealed 154 different variants of which 25 have not been previously reported in a database. In patients without a disease-causing mutation, common genetic variants were detected in a high number of cases, indicating that these common variants may contribute to cholestasis development.
背景与目的
胆盐输出泵(BSEP,ABCB11)、多药耐药蛋白 3(MDR3,ABCB4)和家族性肝内胆汁淤积症 1 型 ATP 酶(FIC1,ATP8B1)介导胆汁形成。本研究旨在确定 FIC1、BSEP 和 MDR3 基因中的突变和常见变异对不同发病和严重程度的胆汁淤积性疾病的贡献。
方法
对具有假定遗传原因的胆汁淤积患者的 ATP8B1、ABCB11 和 ABCB4 基因的编码外显子及其侧翼内含子区域进行测序。通过生物信息学工具和 3D 蛋白建模评估新变异的影响。
结果
在 427 名疑似遗传性胆汁淤积症患者中,分别有 149 名患者在 FIC1、BSEP 或 MDR3 中携带至少一种致病突变。总共发现了 154 种不同的突变,其中 25 种是新的。根据生物信息学分析和同源建模,所有 13 种新型错义突变均为致病性突变。至少有一种致病突变的 82%的患者为儿童。在没有各自基因致病突变的患者中,FIC1 中有 35.3%、BSEP 中有 64.3%和 MDR3 中有 72.6%发现了 1 个或多个常见多态性。与一般人群相比,我们队列中 BSEP 和 MDR3 常见多态性的次要等位基因频率在我们的队列中有所不同,正如 gnomAD 所描述的那样。然而,不同的种族背景可能导致这种影响。
结论
在一个大型患者队列中,在 FIC1、BSEP 和 MDR3 中检测到 154 种不同的变异,其中 25 种是新的。在我们的队列中,BSEP(p.V444A)和 MDR3(p.I237I)多态性的风险等位基因频率在没有各自基因致病突变的患者中显著升高,表明这些常见变异可能导致胆汁淤积表型。
要点总结
FIC1、BSEP 和 MDR3 是胆汁形成所必需的肝胆转运蛋白。这些转运蛋白的遗传变异是广泛的胆汁淤积性肝病的基础。为了确认这些基因对患者表型的遗传贡献,对这三个主要的胆汁淤积相关基因进行了测序,结果在 427 名患者中发现了 154 种不同的变异,其中 25 种尚未在数据库中报道。在没有致病突变的患者中,在大量病例中检测到常见的遗传变异,表明这些常见变异可能导致胆汁淤积的发生。
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