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本文引用的文献

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Characteristics and prevalence of Wilson's disease: A 2013 observational population-based study in France.威尔逊病的特征与患病率:2013年法国一项基于人群的观察性研究。
Clin Res Hepatol Gastroenterol. 2018 Feb;42(1):57-63. doi: 10.1016/j.clinre.2017.05.011. Epub 2017 Jun 23.
2
Carrier frequency of Wilson's disease in the Korean population: a DNA-based approach.韩国人群Wilson 病的载频:一种基于 DNA 的方法。
J Hum Genet. 2017 Sep;62(9):815-818. doi: 10.1038/jhg.2017.49. Epub 2017 May 18.
3
Recommendations for reporting of secondary findings in clinical exome and genome sequencing, 2016 update (ACMG SF v2.0): a policy statement of the American College of Medical Genetics and Genomics.临床外显子组和基因组测序中次要发现报告的建议,2016年更新版(美国医学遗传学与基因组学学会次要发现v2.0):美国医学遗传学与基因组学学会政策声明
Genet Med. 2017 Feb;19(2):249-255. doi: 10.1038/gim.2016.190. Epub 2016 Nov 17.
4
Bioavailable Trace Metals in Neurological Diseases.神经疾病中的生物可利用痕量金属
Curr Treat Options Neurol. 2016 Oct;18(10):46. doi: 10.1007/s11940-016-0426-1.
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Novel mutations of the ATP7B gene in Han Chinese families with pre-symptomatic Wilson's disease.中国汉族早发Wilson 病家系 ATP7B 基因突变研究
World J Pediatr. 2015 Aug;11(3):255-60. doi: 10.1007/s12519-015-0031-5. Epub 2015 Aug 8.
6
Relative exchangeable copper: a promising tool for family screening in Wilson disease.相对可交换铜:肝豆状核变性家系筛查的一种有前景的工具。
Mov Disord. 2014 Apr;29(4):558-62. doi: 10.1002/mds.25763. Epub 2013 Dec 27.
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Disorders of heavy metals.重金属紊乱
Handb Clin Neurol. 2014;120:851-64. doi: 10.1016/B978-0-7020-4087-0.00057-7.
8
Genetically confirmed Wilson disease in a 9-month old boy with elevations of aminotransferases.一名9个月大的男童经基因确诊为威尔逊病,伴有转氨酶升高。
World J Hepatol. 2013 Mar 27;5(3):156-9. doi: 10.4254/wjh.v5.i3.156.
9
A genetic study of Wilson's disease in the United Kingdom.英国的威尔逊病遗传研究。
Brain. 2013 May;136(Pt 5):1476-87. doi: 10.1093/brain/awt035. Epub 2013 Mar 21.
10
Molecular analysis of Wilson patients: direct sequencing and MLPA analysis in the ATP7B gene and Atox1 and COMMD1 gene analysis.Wilson 病患者的分子分析:ATP7B 基因的直接测序和 MLPA 分析,以及 Atox1 和 COMMD1 基因分析。
J Trace Elem Med Biol. 2012 Jun;26(2-3):97-101. doi: 10.1016/j.jtemb.2012.04.024. Epub 2012 Jun 5.

法国威尔逊病的高基因携带者频率:与临床患病率的差异

High genetic carrier frequency of Wilson's disease in France: discrepancies with clinical prevalence.

作者信息

Collet Corinne, Laplanche Jean-Louis, Page Justine, Morel Hélène, Woimant France, Poujois Aurélia

机构信息

Department of Biochemistry and Molecular Biology, Lariboisiere University Hospital, APHP, 2 rue Ambroise Paré, 75010, Paris, France.

INSERM U1132, University Paris-Diderot and Department of Rheumatology, Lariboisiere University Hospital, Paris, France.

出版信息

BMC Med Genet. 2018 Aug 10;19(1):143. doi: 10.1186/s12881-018-0660-3.

DOI:10.1186/s12881-018-0660-3
PMID:30097039
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6086069/
Abstract

BACKGROUND

Wilson's disease (WD) is a rare autosomal recessive metabolic disease caused by ATP7B gene mutations tat cause excessively high copper levels, particularly in the liver and brain. The WD phenotype varies in terms of its clinical presentation and intensity. Diagnosing this metabolic disorder is important as a lifelong treatment, based on the use of copper chelating agents or zinc salts, is more effective if it's started early. Worldwide prevalence of WD is variable, with an average of 1/30,000. In France, a recent study based on French health insurance data estimated the clinical prevalence of the disease to be around 3/200,000.

METHODS

To estimate the genetic prevalence of WD in France, we analysed the ATP7B gene by Next Generation Sequencing from a large French cohort of indiscriminate subjects.

RESULTS

We observed a high heterozygous carrier frequency of ATP7B in France. Among the 697 subjects studied, 18 variants classified as pathogenic or probably pathogenic were found at heterozygous level in 22 subjects (22 alleles/1394 alleles), yielding a prevalence of 0.032 or 1/31 subjects.

CONCLUSIONS

This considerable and unexplained discrepancy between the heterozygous carrier frequency and the clinical prevalence of WD may be explained by the clinical variability, the incomplete penetrance and the existence of modifiers genes. It suggests that the molecular analysis of ATP7B should be interpreted with caution, always alongside copper assays (ceruloplasmin, relative exchangeable copper, 24 h-urinary copper excretion) with particular respect to exome sequencing.

摘要

背景

威尔逊病(WD)是一种罕见的常染色体隐性代谢疾病,由ATP7B基因突变引起,该突变导致铜水平过高,尤其是在肝脏和大脑中。WD的表型在临床表现和严重程度方面存在差异。诊断这种代谢紊乱很重要,因为基于铜螯合剂或锌盐的终身治疗如果早期开始会更有效。WD在全球的患病率各不相同,平均为1/30000。在法国,最近一项基于法国医疗保险数据的研究估计该疾病的临床患病率约为3/200000。

方法

为了估计法国WD的基因患病率,我们通过下一代测序对一大群法国随机受试者的ATP7B基因进行了分析。

结果

我们在法国观察到ATP7B基因的杂合子携带频率很高。在研究的697名受试者中,在22名受试者(22个等位基因/1394个等位基因)的杂合子水平上发现了18个被分类为致病或可能致病的变体,患病率为0.032或1/31受试者。

结论

WD杂合子携带频率与临床患病率之间这种显著且无法解释的差异可能由临床变异性、不完全外显率和修饰基因的存在来解释。这表明对ATP7B的分子分析应谨慎解释,始终要结合铜检测(铜蓝蛋白、相对可交换铜、24小时尿铜排泄),尤其是在外显子测序方面。