Cox D W, Prat L, Walshe J M, Heathcote J, Gaffney D
Department of Medical Genetics, University of Alberta, Edmonton, Alberta, Canada.
Hum Mutat. 2005 Sep;26(3):280. doi: 10.1002/humu.9358.
Wilson disease (WND), an autosomal recessive disorder of copper transport, shows wide genotypic and phenotypic variability, with hepatic and/or neurological symptoms. The WND gene, ATP7B, encodes a copper transporting ATPase that is involved in the transport of copper into the plasma protein ceruloplasmin, and in the excretion of copper from the liver. ATP7B mutations result in copper storage in liver and brain. From 247 WND patients worldwide whose DNA has been sequenced in our laboratory, we have identified 24 new mutations. The origins of the patients were European white (one deletion, one nonsense, one splice site, and 18 missense), Chinese (one deletion, one missense) and Bangladeshi (one missense). Most of these had strong support as disease causing mutations, based on conservation between species, structural changes, and absence in controls. One missense mutation in a Chinese patient was considered uncertain because of its conservative nature and position in the protein. We also identified 15 nucleotide substitutions (11 of them new) causing silent or intronic changes, none of which produce an additional splice site that could lead to disease. Characterization of mutations, both disease-causing and normal variants, is essential for accurate molecular diagnosis of this condition.
威尔逊病(WND)是一种常染色体隐性铜转运障碍疾病,具有广泛的基因型和表型变异性,伴有肝脏和/或神经症状。WND基因ATP7B编码一种铜转运ATP酶,该酶参与铜向血浆蛋白铜蓝蛋白的转运以及肝脏中铜的排泄。ATP7B突变导致铜在肝脏和大脑中蓄积。在我们实验室对全球247例已进行DNA测序的WND患者中,我们鉴定出24个新突变。患者来源包括欧洲白人(1个缺失突变、1个无义突变、1个剪接位点突变和18个错义突变)、中国人(1个缺失突变、1个错义突变)和孟加拉人(1个错义突变)。基于物种间的保守性、结构变化以及在对照中未出现,这些突变中的大多数有充分证据支持其为致病突变。一名中国患者的一个错义突变因其保守性质和在蛋白质中的位置而被认为不确定。我们还鉴定出15个导致沉默或内含子变化的核苷酸替换(其中11个是新发现的),这些变化均未产生可导致疾病的额外剪接位点。对致病突变和正常变异进行特征分析对于准确分子诊断该疾病至关重要。
