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Mutation Detection in the Menkes Gene ATP7A Using the Protein Truncation Test

机译:使用蛋白质截断测试检测Menkes基因ATP7A中的突变

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摘要

Menkes disease (MD) is a rare recessively inherited lethal disorder of copper metabolism. The gene ATP7A defective in MD consists of 23 exons and the coding region encompasses 4500 bp. About 300 distinct mutations, representing all types, have been identified in ATP7A. However all mutations identified so far in the exon 2 to exon 7, corresponding to 1869 bp of the coding sequence, result in truncated protein products. No missense mutations have been identified in this region. As about 30% of the total number of mutations identified are located in exon 2 to exon 7, we have designed a protein truncation test (PTT) for rapid detecting of mutations in this part of the gene. In order to determine the applicability of the test, we analysed RNA obtained from eleven MD patients with known mutations in this region. As a truncated product could be identified in all the included samples, PTT proves to be a useful technique for rapid detection of mutations in the N-terminal part of the ATP7A gene. Furthermore as MD is a X-linked disease, normally only affecting boys, the risk of false negative results, due to nonsense mediated RNA decay, leading to allelic exclusion, can be left out of account.
机译:Menkes病(MD)是一种罕见的隐性遗传性铜代谢潜伏性疾病。 MD中的ATP7A缺陷基因由23个外显子组成,编码区涵盖4500 bp。在ATP7A中已鉴定出约300种代表所有类型的独特突变。但是,到目前为止,在外显子2至外显子7中鉴定到的所有突变(对应于编码序列的1869 bp)均导致蛋白产物被截断。在该区域没有发现错义突变。由于鉴定出的突变总数中约30%位于第2外显子至第7外显子,我们设计了一种蛋白质截短测试(PTT),用于快速检测该基因部分的突变。为了确定该测试的适用性,我们分析了从11名在该区域具有已知突变的MD患者获得的RNA。由于可以在所有包含的样品中鉴定出截短的产物,因此PTT被证明是一种用于快速检测ATP7A基因N端突变的有用技术。此外,由于MD是一种X连锁疾病,通常仅影响男孩,因此可以忽略由于无意义介导的RNA衰变而导致等位基因排斥的假阴性结果风险。

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