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The PSP-associated MAPT H1 subhaplotype in Guadeloupean atypical parkinsonism.

机译:瓜德罗普岛非典型帕金森病患者中与PSP相关的MAPT H1亚型。

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The aim of this study was to determine whether the H1 subhaplotype in MAPT associated with progressive supranuclear palsy (PSP) in Caucasians confers risk for PSP-like atypical parkinsonism in Guadeloupe, a tauopathy. Guadeloupean controls and patients with atypical and idiopathic parkinsonism and ethnically and age-matched controls were genotyped for H1 and H2 alleles, then for the H1 subhaplotype associated with PSP in Caucasians, using previously described haplotype-tagging single nucleotide polymorphisms (Ht-SNPs) in linkage disequilibrium at the MAPT locus. Most Guadeloupean controls and patients were homozygous for the H1 allele; only 5% were heterozygous for the H2 allele, consistent with the European contribution to the racial admixture in Guadeloupe, but equivalent to the frequency found in Caucasian PSP patients. The frequencies of the Ht-SNPs used to determine the PSP-associated H1 subhaplotype in both Guadeloupean controls and parkinsonians were similar, indicating that the H1 subhaplotype associated with PSP in Caucasians was not a risk factor for PSP-like atypical parkinsonism in Guadeloupe. Interestingly, they were also similar to the frequencies in Caucasian PSP patients. The major H1 subhaplotype in Guadeloupe, determined by analysis of linkage desequibrium, differed from the major Caucasian subhaplotype, but corresponded to minor alleles previously described.
机译:这项研究的目的是确定高加索人的MAPT中H1亚型与进行性核上性麻痹(PSP)相关是否赋予患tauopathy的瓜德罗普岛PSP样非典型帕金森病风险。使用先前描述的单倍型标记单核苷酸多态性(Ht-SNPs),将瓜德罗普岛的对照人群,非典型和特发性帕金森病患者以及种族和年龄匹配的对照人群的H1和H2等位基因进行基因分型,然后对与PSP相关的H1亚型进行基因分型。 MAPT基因座处的连锁不平衡。大多数瓜德罗普岛对照和患者的H1等位基因是纯合的。 H2等位基因只有5%杂合,这与欧洲对瓜德罗普岛种族混合的贡献一致,但与白种人PSP患者中发现的频率相同。用于确定瓜德罗普岛对照和帕金森病患者中与PSP相关的H1亚型的Ht-SNP的频率相似,表明高加索人中与PSP相关的H1亚型不是瓜德罗普岛中类似PSP的非典型帕金森病的危险因素。有趣的是,它们也与白种人PSP患者的频率相似。瓜德罗普岛的主要H1亚型通过连锁不平衡分析确定,不同于主要的白种人亚型,但对应于先前描述的次要等位基因。

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