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Molecular analysis of lipoid proteinosis: identification of a novel nonsense mutation in the ECM1 gene in a Pakistani family

机译:脂质蛋白沉着症的分子分析:巴基斯坦家庭ECM1基因中的一个新的无意义突变的鉴定。

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Lipoid proteinosis is a rare autosomal recessive disease characterized by cutaneous and mucosal lesions and hoarseness appearing in early childhood that is caused by homozygous or compound heterozygous mutations in the ECM1 gene located on chromosome 1q21. The aim of the study was to investigate the molecular genetic defect underlying lipoid proteinosis in a consanguineous Pakistani family. Methods Genotyping of seven members of the family was performed by amplifying microsatellite markers, tightly linked to the ECM1 gene. To screen for mutations in the ECM1 gene, all of its exons and splice junctions were PCR amplified from genomic DNA and analyzed by SSCP and sequenced directly in an ABI 3130 genetic analyzer. Results The results revealed linkage of the LP family to the ECM1 locus. Sequence analysis of the coding exons and splice junctions of the ECM1 gene revealed a novel homozygous mutation (c.616C > T) in exon 6, predicted to replace glutamine with stop codon (p.Q206X) at amino acid position 206. Conclusions The finding of a novel mutation in Pakistani family extends the body of evidence that supports the importance of ECM1 gene for the development of lipoid proteinosis.
机译:类脂蛋白沉着病是一种罕见的常染色体隐性遗传疾病,其特征是在儿童早期出现的皮肤和粘膜病变以及声音嘶哑,这是由位于染色体1q21上的ECM1基因的纯合子或复合杂合子突变引起的。这项研究的目的是调查近亲巴基斯坦家庭中类脂蛋白沉着症的分子遗传缺陷。方法通过扩增与ECM1基因紧密相连的微卫星标记,对7个家庭成员进行基因分型。为了筛选ECM1基因中的突变,从基因组DNA中扩增了其所有外显子和剪接点,并通过SSCP分析,并在ABI 3130遗传分析仪中直接测序。结果结果表明,LP家族与ECM1基因座相关。对ECM1基因编码外显子和剪接点的序列分析显示,外显子6中有一个新的纯合突变(c.616C> T),预计在氨基酸206位用终止密码子(p.Q206X)代替谷氨酰胺。结论家族中一个新突变的发现扩展了支持ECM1基因对类脂蛋白病发展的重要性的证据。

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