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Pathogenicity of Intronic and Synonymous Variants of ATP7B in Wilson Disease

小基因 RNA剪接 生物 遗传学 生物信息学 致病性 内含子 突变 疾病 表型 基因 核糖核酸 医学 内科学 微生物学
作者
Wan‐Qing Xu,Rou‐Min Wang,Yi Dong,Zhi‐Ying Wu
出处
期刊:The Journal of Molecular Diagnostics [Elsevier BV]
卷期号:25 (1): 57-67 被引量:10
标识
DOI:10.1016/j.jmoldx.2022.10.002
摘要

Wilson disease (WD) is a hereditary disorder of copper metabolism, resulting from mutations within ATP7B. Early diagnosis is essential for affected individuals. However, there are still patients with clinically suspected WD who do not have detectable pathogenic variants, which makes diagnosis difficult and delays treatment. This study included such patients from the authors' center and screened for the full-length sequence of ATP7B by next-generation sequencing. Newly identified synonymous and intronic variants were then analyzed with in silico tools. A minigene system was constructed to determine the pathogenicity of these variants in terms of splicing and blood RNA extraction, and RT-PCR experiments were performed on several patients to verify the splicing alterations. The phenotypes of the patients were also analyzed. Fourteen suspected pathogenic variants, including nine synonymous and five intronic variants, were detected in 12 patients with clinically suspected WD. Among them, four synonymous variants (c.1050G>A, c.1122C>G, c.3243G>A, and c.4014T>A) and four intronic variants (c.1543 +40G>A, c.1707+6_1707+16del, c.1870-49A>G, and c.2731-67A>G) resulted in splicing changes in ATP7B. After the above analysis, the diagnosis of WD could be confirmed in eight clinically suspected patients with WD who showed a late age of onset.
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