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Characterization and localization of human COX17, a gene involved in mitochondrial copper transport.

机译:人COX17的特征和定位,该基因涉及线粒体铜转运。

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Deficiencies in cytochrome oxidase (COX), the terminal enzyme of the mitochondrial respiratory chain, are relatively rare but most often lethal. The underlying causes are beginning to be elucidated, and most mutations are thought to affect the function of proteins involved in assembling the holoenzyme. COX17 is such an assembly protein and is thought to recruit copper to mitochondria for incorporation into the COX apoenzyme. Here we present the gene structure, the expression, and chromosomal localization for COX17, a candidate gene for COX deficiency. The COXI 7 gene spans approximately 8 kb of human genomic DNA and encodes a transcript of approximately 450 bp that is expressed in all tissues tested. Although the COX17 gene was previously mapped to chromosome 13q14-21, our results suggest that a COX17 pseudogene maps to this region. The pseudogene contains several nucleotide changes, including one that would result in an altered amino acid in the putative copper binding domain. We have localized the gene encoding the COX 17 protein to the long arm of chromosome 3 by radiation hybrid mapping. Deciphering of the COX17 genomic structure will allow this gene to be assessed for mutations in COX deficient patients.
机译:线粒体呼吸链末端酶细胞色素氧化酶(COX)的缺乏相对罕见,但最致命。开始阐明其根本原因,并且认为大多数突变会影响组装全酶的蛋白质的功能。 COX17是一种装配蛋白,被认为可以将铜募集到线粒体中以整合到COX脱辅酶中。在这里,我们介绍了COX17(COX缺乏症的候选基因)的基因结构,表达和染色体定位。 COXI 7基因跨越人类基因组DNA的大约8 kb,并编码在所有测试的组织中表达的大约450 bp的转录本。尽管以前将COX17基因定位到13q14-21号染色体,但我们的结果表明,COX17假基因定位于该区域。该假基因包含几个核苷酸变化,包括一个可能导致推定的铜结合域中氨基酸发生改变的变化。我们已经通过辐射杂交作图将编码COX 17蛋白的基因定位在3号染色体的长臂上。对COX17基因组结构的解密将使该基因可以评估COX缺乏症患者的突变。

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