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首页> 外文期刊>Parkinsonism & related disorders >Genetic screening for mutations in the Nrdp1 gene in Parkinson disease patients in a Chinese population.
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Genetic screening for mutations in the Nrdp1 gene in Parkinson disease patients in a Chinese population.

机译:对中国人群帕金森病患者Nrdp1基因突变的遗传筛查。

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摘要

Strong evidence has shown that a defect in the Parkin gene is known to be a common, genetic cause of Parkinson disease (PD). The E3 ubiquitin ligase Nrdp1 is shown to interact with the N terminal of Parkin (the first 76 amino acids) and catalyze degradation of Parkin via the ubiquitin-proteasome pathway, suggesting that Nrdp1 may be involved in the development of PD via the regulation of Parkin, We believe we are the first to have screened PD patients for mutations in the Nrdp1 gene to determine the association between these variants and PD. By direct sequencing, we analysed the entire coding regions and 5' UTR of Nrdp1 in 209 Chinese PD patients and 302 unrelated healthy individuals. No variant was detected in the coding regions (exons 3-7); only 2 variants (c.-206 T > A and c.-208-8 A > G) were identified in the 5' UTR (exon 2) and intron 1. Furthermore, a study of the allelic and genotypic association between patients and controls showed no significant association between the c.-206 T > A polymorphism and PD; c.-208-8 A > G was identified in one PD patient and not in controls. Our data do not support the hypothesis of a major role for the Nrdp1 gene in PD development in the Chinese population.
机译:有力的证据表明,已知帕金基因的缺陷是帕金森病(PD)的常见遗传原因。 E3泛素连接酶Nrdp1已显示与Parkin的N末端(前76个氨基酸)相互作用,并通过泛素-蛋白酶体途径催化Parkin的降解,这表明Nrdp1可能通过调节Parkin参与PD的发展。 ,我们相信我们是第一个针对PD患者筛查Nrdp1基因突变的方法,以确定这些变体与PD之间的关联。通过直接测序,我们分析了209名中国PD患者和302名无关健康个体的Nrdp1的整个编码区和5'UTR。在编码区未检测到变体(外显子3-7);在5'UTR(第2外显子)和内含子1中仅鉴定出2个变体(c.-206 T> A和c.-208-8 A> G)。此外,对患者和患者之间等位基因和基因型关联的研究对照显示c.-206 T> A多态性与PD之间无显着相关性。 c.-208-8在一名PD患者中而非对照组中发现了A>G。我们的数据不支持Nrdp1基因在中国人群PD发育中起主要作用的假设。

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