| Translational Neurodegeneration | |
| Clinical and genetic characterization of a large cohort of patients with Wilson’s disease in China | |
| Xiang Li1 Jing Zhang1 Pei Pei1 Ting Dong1 Wenming Yang2 Yue Yang2 Shijie Zhang3 | |
| [1] Department of Neurology, The First Affiliated Hospital of Anhui University of Chinese Medicine, 230031, Hefei, China;Department of Neurology, The First Affiliated Hospital of Anhui University of Chinese Medicine, 230031, Hefei, China;Key Laboratory of Xin’An Medicine, Anhui University of Chinese Medicine, 230031, Hefei, China;Experimental Center of Clinical Research, The First Affiliated Hospital of Anhui University of Chinese Medicine, 230031, Hefei, China; | |
| 关键词: Wilson’s disease; Chinese; ATP7B; Genotype–phenotype correlation; Large cohort study; | |
| DOI : 10.1186/s40035-022-00287-0 | |
| 来源: Springer | |
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【 摘 要 】
BackgroundWilson’s disease (WD) is an autosomal recessive disorder of copper metabolism caused by ATP7B (encoding a copper-transporting P-type ATPase) variants that shows various characteristics according to race and geographical region. This study was aimed to provide a comprehensive analysis of ATP7B variants in China and to investigate a plausible role of common variants in WD manifestations.MethodsA total of 1366 patients (1302 index patients and 64 siblings) clinically diagnosed with WD (Leipzig score ≥ 4) were recruited. They underwent ATP7B gene sequencing and information of age and symptoms at onset was collected. The genotype–phenotype correlation was assessed in the index patients who were examined with two pathogenic variants and onset with hepatic (n = 276) or neurologic (n = 665) symptoms.ResultsWe identified 294 potentially pathogenic ATP7B variants (112 truncating, 174 missense, 8 in-frame) in the 1302 index patients, including 116 novel variants. The most frequent variant was c.2333G>T (R778L, allele frequency: 28.96%), followed by c.2975C>T (P992L, 13.82%), c.2621C>T (A874V, 5.99%), c.2755C>G (R919G, 2.46%), and c.3646G>A (V1216M, 1.92%). In 1167 patients, both pathogentic variants were identified, of which 532 different variant combinations were found. By binary logistic regression analysis, the factor associated with neurological presentation was high age-at-onset, but not sex, protein-truncating variant (PTV), or the common missense variants (R778L, P992L, and A874V). In the neurological group, low age-at-onset was a factor associated with dystonia, gait abnormality, and salivation; high age-at-onset was a factor associated with tremor; and the sex, low age-at-onset and A874V were independent factors associated with dysarthria. In addition, PTV, R778L, and P992L were predominant in early-onset patients, whereas A874V was predominant in late-onset patients, and patients with R778L/A874V genotype displayed a higher age-at-onset than patients with R778L/R778L or R778L/P992L genotype.ConclusionsOur work expanded the ATP7B variant spectrum and highlighted the differences among patients with WD in age-at-onset and ATP7B variants, which may provide some valuable insights into the diagnosis, counseling, and treatment of patients with WD.
【 授权许可】
CC BY
【 预 览 】
| Files | Size | Format | View |
|---|---|---|---|
| RO202202181720190ZK.pdf | 4400KB |  download |
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