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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Aberrant splicing and truncated-protein expression due to a newly identified XPA gene mutation.
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Aberrant splicing and truncated-protein expression due to a newly identified XPA gene mutation.

机译:由于新发现的XPA基因突变,导致异常剪接和截短蛋白表达。

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摘要

A group A xeroderma pigmentosum (XPA) patient, XP2NI, is a compound heterozygote with a newly identified G to C transversion at the last nucleotide in exon 5 in one chromosome, and with the known splicing mutation in intron 3 in another chromosome in the XPA gene. XP2NI had mild skin symptoms and the cells were slightly less sensitive to UV radiation than the cells of typical severe XPA patients who have the splicing mutation in intron 3 homozygously. Reverse transcriptase (RT)-PCR and sequencing of the PCR products revealed that the mutation in exon 5 resulted in producing three types of aberrant mRNA, lacking 7 nucleotides at the end of exon 5, lacking entire exon 5, and lacking exons 3, 4 and 5. A significant amount of a truncated type of protein was produced in XP2NI cells, and the size of the protein indicated that it should have been translated from the mRNA, lacking the 7 nucleotides and retained one of the zinc-finger domains required for the DNA repair activity. The clinical mildness of XP2NI may be due to the residual DNA repair activity of the truncated XPA protein, while no XPA protein was detected in the XPA cells with the homozygous intron 3 splicing mutation.
机译:一组干性色素性皮肤病(XPA)患者XP2NI是一种复合杂合子,在一个染色体的第5外显子的最后一个核苷酸处具有新鉴定的G到C转换,并且在XPA的另一个染色体中具有内含子3的已知剪接突变。基因。 XP2NI具有轻度的皮肤症状,其细胞对紫外线辐射的敏感性略低于纯合内含子3中具有剪接突变的典型严重XPA患者的细胞。逆转录酶(RT)-PCR和PCR产物测序表明,外显子5的突变导致产生三种类型的异常mRNA,在外显子5的末端缺少7个核苷酸,缺少完整的外显子5,并且缺少外显子3、4 5.在XP2NI细胞中产生了大量的截短型蛋白质,该蛋白质的大小表明它应该已经从mRNA中翻译出来,缺少7个核苷酸,并保留了所需的一个锌指结构域。 DNA修复活性。 XP2NI的临床温和性可能是由于截短的XPA蛋白具有残留的DNA修复活性,而纯合内含子3剪接突变的XPA细胞中未检测到XPA蛋白。

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