[Genotype-phenotype relationship and genetics study of 115 cases with Wilson's disease].

J K Xia, H F Ning, X Luo, Y Zeng, Y B Chen, X D Kong
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Abstract

Objective: To explore the genotype-phenotype relationship of Wilson's disease (WD) and further study the mutation spectrum in the ATP7B gene. Methods: The clinical data and genetic test results of 115 cases with WD diagnosed in the First Affiliated Hospital of Zhengzhou University from 2015 to 2022 were retrospectively analyzed. The rank sum test was used for quantitative data comparison, and χ(2) test was used for count data comparison. Multivariate logistic regression was used to analyze the relationship between patients' genotype and phenotype. Results: The onset of liver manifestations (hepatic type) accounted for 60.9%, neurological symptoms (cerebral type) for 13.0%, and mixed hepato-cerebral symptoms for 26.1%. Presymptomatic individuals (hepatic types) accounted for 62.9%. Next-generation sequencing- diagnosed WD cases accounted for 87.8%. Combined multiplex ligation-dependent probe amplification assay-diagnosed WD cases accounted for 89.6%. A single case with a detected pathogenic locus accounted for 10.4%. The diagnostic rate of WD by genetic testing combined with clinical data was 100%. A total of 76 ATP7B mutations were detected, and the top three mutation frequencies were c.2333G>T (p.Arg778Leu) (30.7%), c.2975C>T (p.Pro992Leu) (7.3%), and c.2621C>T (p.Ala874Val) (6.4%). The mutations were mainly distributed in exons 8, 11-13, and 15-18, accounting for more than 90% of the total mutations. Eight new mutations were found, including c.3724G>A (p.Glu1242Lys), c.3703G>C (p.Gly1235Arg), c.3593T>C (p.Val1198Ala), c.2494A>C (p.Lys832Gln), c.1517T>A (p.Ile506Lys), c.484G>T (p.Glu162Ter), c.1870-49A>G, and the missing of exons 10-21. Liver histopathology showed cellular edema, degeneration, inflammation, and necrosis, as well as a 42.8% copper staining positive rate. Genotype-phenotype analysis showed that the p.Arg778Leu mutation had higher alanine aminotransferase (ALT) levels than those carrying other mutations (P=0.024), while the homozygous mutation of p.Arg778Leu was associated with cerebral-type patients (P=0.027). Conclusion: Genetic testing plays an important role in the diagnosis of WD. p.Arg778Leu is the first high-frequency mutation in the Chinese population, and patients carrying it have higher ALT levels. The p.Arg778Leu homozygous mutation is prone to causing cerebral-type WD. This study expands the ATP7B gene mutation spectrum.

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[115例威尔逊氏病患者的基因型-表型关系和遗传学研究]。
研究目的探讨威尔逊氏病(WD)的基因型与表型关系,并进一步研究 ATP7B 基因的突变谱。方法回顾性分析郑州大学第一附属医院2015年至2022年确诊的115例WD患者的临床资料和基因检测结果。定量数据比较采用秩和检验,计数数据比较采用χ(2)检验。采用多元Logistic回归分析患者基因型与表型之间的关系。结果肝脏症状(肝型)占 60.9%,神经症状(脑型)占 13.0%,肝脑混合症状占 26.1%。无症状者(肝型)占 62.9%。经新一代测序确诊的 WD 病例占 87.8%。联合多重连接依赖探针扩增分析确诊的 WD 病例占 89.6%。检测到致病基因位点的单个病例占 10.4%。通过基因检测结合临床数据对 WD 的诊断率为 100%。共检测到76个ATP7B基因突变,突变频率最高的三个基因分别为c.2333G>T (p.Arg778Leu) (30.7%)、c.2975C>T (p.Pro992Leu) (7.3%)和c.2621C>T (p.Ala874Val) (6.4%)。突变主要分布在第 8、11-13 和 15-18 号外显子,占突变总数的 90% 以上。发现了 8 个新的突变,包括 c.3724G>A(p.Glu1242Lys)、c.3703G>C(p.Gly1235Arg)、c.3593T>C(p.Val1198Ala)、c.2494A>C(p.Lys832Gln)、c.1517T>A(p.Ile506Lys)、c.484G>T(p.Glu162Ter)、c.1870-49A>G,以及外显子 10-21 缺失。肝脏组织病理学显示细胞水肿、变性、炎症和坏死,铜染色阳性率为 42.8%。基因型-表型分析显示,p.Arg778Leu突变者的丙氨酸氨基转移酶(ALT)水平高于其他突变者(P=0.024),而p.Arg778Leu的同源突变与脑型患者有关(P=0.027)。结论p.Arg778Leu是中国人群中首个高频突变,携带该突变的患者ALT水平较高。p.Arg778Leu同源突变易导致脑型WD。这项研究扩展了ATP7B基因突变谱。
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来源期刊
中华肝脏病杂志
中华肝脏病杂志 Medicine-Medicine (all)
CiteScore
1.20
自引率
0.00%
发文量
7574
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