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Re-evaluation of the diagnostic criteria for Wilson disease in children with mild liver disease.重新评估小儿轻度肝病时 Wilson 病的诊断标准。
Hepatology. 2010 Dec;52(6):1948-56. doi: 10.1002/hep.23910. Epub 2010 Oct 21.
2
Truncating mutations in the Wilson disease gene ATP7B are associated with very low serum ceruloplasmin oxidase activity and an early onset of Wilson disease.威尔逊病基因 ATP7B 中的截断突变与极低的血清铜蓝蛋白氧化酶活性和威尔逊病的早期发病有关。
BMC Gastroenterol. 2010 Jan 18;10:8. doi: 10.1186/1471-230X-10-8.
3
Serum ceruloplasmin oxidase activity is a sensitive and highly specific diagnostic marker for Wilson's disease.血清铜蓝蛋白氧化酶活性是肝豆状核变性的一种敏感且高度特异的诊断标志物。
J Hepatol. 2009 Nov;51(5):925-30. doi: 10.1016/j.jhep.2009.06.022. Epub 2009 Jul 30.
4
Molecular diagnosis of Menkes disease: genotype-phenotype correlation.门克斯病的分子诊断:基因型与表型的相关性
Biochimie. 2009 Oct;91(10):1273-7. doi: 10.1016/j.biochi.2009.05.011. Epub 2009 Jun 6.
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Translational read-through of a nonsense mutation in ATP7A impacts treatment outcome in Menkes disease.ATP7A基因无义突变的翻译通读影响门克斯病的治疗结果。
Ann Neurol. 2009 Jan;65(1):108-13. doi: 10.1002/ana.21576.
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CPT2 gene mutations resulting in lethal neonatal or severe infantile carnitine palmitoyltransferase II deficiency.导致致死性新生儿或严重婴儿型肉碱棕榈酰转移酶II缺乏症的CPT2基因突变。
Mol Genet Metab. 2008 Aug;94(4):422-427. doi: 10.1016/j.ymgme.2008.05.002. Epub 2008 Jun 11.
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Diagnosis and treatment of Wilson disease: an update.威尔逊病的诊断与治疗:最新进展
Hepatology. 2008 Jun;47(6):2089-111. doi: 10.1002/hep.22261.
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Distinct Wilson's disease mutations in ATP7B are associated with enhanced binding to COMMD1 and reduced stability of ATP7B.ATP7B基因中不同的威尔逊氏病突变与增强的COMMD1结合及ATP7B稳定性降低相关。
Gastroenterology. 2007 Oct;133(4):1316-26. doi: 10.1053/j.gastro.2007.07.020. Epub 2007 Jul 25.
9
Re-evaluation of the penicillamine challenge test in the diagnosis of Wilson's disease in children.儿童威尔逊病诊断中青霉胺激发试验的重新评估
J Hepatol. 2007 Aug;47(2):270-6. doi: 10.1016/j.jhep.2007.03.011. Epub 2007 Apr 4.
10
Clinical and molecular characterization of Wilson disease in Spanish patients.西班牙Wilson 病患者的临床和分子特征。
Hepatol Res. 2007 Jan;37(1):18-26. doi: 10.1111/j.1872-034X.2007.00010.x.

丹麦威尔逊病患者的临床表现和突变。

Clinical presentation and mutations in Danish patients with Wilson disease.

机构信息

Kennedy Center, Department of Human Molecular Genetics, Gl. Landevej 7,Glostrup, Denmark.

出版信息

Eur J Hum Genet. 2011 Sep;19(9):935-41. doi: 10.1038/ejhg.2011.80. Epub 2011 May 25.

DOI:10.1038/ejhg.2011.80
PMID:21610751
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3179371/
Abstract

This study describes the clinical presentation and diagnosis in all Danish patients (49, 41 unrelated) with Wilson disease (WND). On the basis of the number of diagnosed patients from 1990-2008, the prevalence was estimated to be 1:49 500. Among routinely used diagnostic tests, none were consistently indicative of WND, with the exception of the 24-h urine-Cu test, which is always outside the normal range. Mutations were identified in 100% of the screened ATP7B alleles (70 unrelated), including five novel mutations: p.1021K; p.G1158V; p.L1304F; IVS20-2A>G; Ex5_6del. In all, 70% of mutations were found in exons 8, 14, 17, 18, and 20. The most frequent mutation, p.H1069Q, comprised 18%. We propose a new and simple model that correlates genotype and age of onset. By assuming that the milder of two mutations is 'functionally dominant' and determines the age of onset, we classified 25/27 mutations as either severe (age of onset <20 years) or moderate (age of onset >20 years), and correctly predicted the age of onset in 37/39 patients. This method should be tested in other Wilson populations.

摘要

本研究描述了所有丹麦患者(49 例非相关患者)的临床表型和诊断。根据 1990-2008 年确诊患者的数量,估计患病率为 1:49500。在常规使用的诊断测试中,没有一项能始终明确提示威尔逊病,除了 24 小时尿铜测试,其结果总是超出正常范围。在筛查的 ATP7B 等位基因(70 例非相关)中,发现了 100%的突变,包括 5 种新突变:p.1021K;p.G1158V;p.L1304F;IVS20-2A>G;Ex5_6del。总共,70%的突变发生在 8、14、17、18 和 20 号外显子中。最常见的突变 p.H1069Q 占 18%。我们提出了一个新的简单模型,将基因型与发病年龄相关联。假设两种突变中较轻的一种是“功能显性”,并决定发病年龄,我们将 25/27 种突变分类为严重(发病年龄<20 岁)或中度(发病年龄>20 岁),并正确预测了 39 例患者中的 37 例发病年龄。这种方法应在其他威尔逊人群中进行测试。