Molecular and computational characterization of ABCB11 and ABCG5 variants in Tunisian patients with neonatal/infantile low-GGT intrahepatic cholestasis: Genetic diagnosis and genotype–phenotype correlation assessment

IF 1 4区 生物学 Q4 GENETICS & HEREDITY
Boudour Khabou, Fakhri Kallabi, Rim Ben Abdelaziz, Ines Maaloul, Hajer Aloulou, Amel ben Chehida, Thouraya Kammoun, Veronique Barbu, Tahya Sellami Boudawara, Faiza Fakhfakh, Bassem Khemakhem, Olfa Siala Sahnoun
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引用次数: 0

Abstract

Many inherited conditions cause hepatocellular cholestasis in infancy, including progressive familial intrahepatic cholestasis (PFIC), a heterogeneous group of diseases with highly overlapping symptoms. In our study, six unrelated Tunisian infants with PFIC suspicion were the subject of a panel–target sequencing followed by an exhaustive bioinformatic and modeling investigations. Results revealed five disease-causative variants including known ones: (the p.Asp482Gly and p.Tyr354 * in the ABCB11 gene and the p.Arg446 * in the ABCC2 gene), a novel p.Ala98Cys variant in the ATP-binding cassette subfamily G member 5 (ABCG5) gene and a first homozygous description of the p.Gln312His in the ABCB11 gene. The p.Gln312His disrupts the interaction pattern of the bile salt export pump as well as the flexibility of the second intracellular loop domain harboring this residue. As for the p.Ala98Cys, it modulates both the interactions within the first nucleotide-binding domain of the bile transporter and its accessibility. Two additional potentially modifier variants in cholestasis-associated genes were retained based on their pathogenicity (p.Gly758Val in the ABCC2 gene) and functionality (p.Asp19His in the ABCG8 gene). Molecular findings allowed a PFIC2 diagnosis in five patients and an unexpected diagnosis of sisterolemia in one case. The absence of genotype/phenotype correlation suggests the implication of environmental and epigenetic factors as well as modifier variants involved directly or indirectly in the bile composition, which could explain the cholestasis phenotypic variability.

突尼斯新生儿/婴幼儿低GGT肝内胆汁淤积症患者ABCB11和ABCG5变体的分子和计算特征:基因诊断和基因型表型相关性评估。
许多遗传性疾病会导致婴儿期肝细胞胆汁淤积症,包括进行性家族性肝内胆汁淤积症(PFIC),这是一组症状高度重叠的异质性疾病。在我们的研究中,对六名怀疑患有 PFIC 的无亲属关系的突尼斯婴儿进行了面板-靶标测序,然后进行了详尽的生物信息学和建模研究。结果发现了五个致病变异体,包括已知的变异体:(ABCB11 基因中的 p.Asp482Gly 和 p.Tyr354 * 以及 ABCC2 基因中的 p.Arg446 *)、ATP 结合盒 G 亚家族成员 5(ABCG5)基因中的新型 p.Ala98Cys 变异体以及 ABCB11 基因中的 p.Gln312His 首次同源描述。p.Gln312His破坏了胆盐输出泵的相互作用模式以及含有该残基的第二个胞内环状结构域的灵活性。至于 p.Ala98Cys,它既改变了胆汁转运体第一个核苷酸结合域内的相互作用,也改变了胆汁转运体的可及性。根据致病性(ABCC2 基因中的 p.Gly758Val)和功能性(ABCG8 基因中的 p.Asp19His),保留了胆汁淤积相关基因中另外两个潜在的修饰变异。分子研究结果使五例患者被诊断为 PFIC2,一例患者被意外诊断为姊妹卵巢血症。基因型/表型之间缺乏相关性,这表明环境和表观遗传因素以及直接或间接参与胆汁组成的修饰变异的影响,可以解释胆汁淤积症的表型变异。
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来源期刊
Annals of Human Genetics
Annals of Human Genetics 生物-遗传学
CiteScore
4.20
自引率
0.00%
发文量
34
审稿时长
3 months
期刊介绍: Annals of Human Genetics publishes material directly concerned with human genetics or the application of scientific principles and techniques to any aspect of human inheritance. Papers that describe work on other species that may be relevant to human genetics will also be considered. Mathematical models should include examples of application to data where possible. Authors are welcome to submit Supporting Information, such as data sets or additional figures or tables, that will not be published in the print edition of the journal, but which will be viewable via the online edition and stored on the website.
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