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Determination of ancestral alleles for human single-nucleotide polymorphisms using high-density oligonucleotide arrays

机译:使用高密度寡核苷酸阵列确定人类单核苷酸多态性的祖先等位基因

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Here we report the application of high-density oligonucleotide array (DNA chip)-based analysis to determine the distant history of single nucleotide polymorphisms (SNPs) in current human populations. We analysed orthologues for 397 human SNP sites (identified in CEPH pedigrees from Amish, Venezuelan and Utah populations) from 23 common chimpanzee, 19 pygmy chimpanzee and 11 gorilla genomic DNA samples. From this data we determined 214 proposed ancestral alleles (the sequence found in the last common ancestor of humans and chimpanzees). In a diverse human population set, we found that SNP alleles with higher frequencies were more likely to be ancestral than less frequently occurring alleles. There were, however, exceptions. We also found three shared human/ pygmy chimpanzee polymorphisms, all involving CpG dinu-cleotides, and two shared human/gorilla polymorphisms, one involving a CpG dinucleotide. We demonstrate that microarray-based assays allow rapid comparative sequence analysis of intra- and interspedes genetic variation.
机译:在这里,我们报告基于高密度寡核苷酸阵列(DNA芯片)的分析的应用,以确定当前人群中单核苷酸多态性(SNP)的遥远历史。我们分析了23个常见黑猩猩,19个侏儒黑猩猩和11个大猩猩基因组DNA样本中397个人类SNP位点的直系同源物(在来自阿米什人,委内瑞拉人和犹他州的CEPH家谱中确定)。从这些数据中,我们确定了214个提议的祖先等位基因(在人类和黑猩猩的最后一个共同祖先中发现的序列)。在一个多样化的人群中,我们发现频率较高的SNP等位基因比不经常出现的等位基因更可能是祖先的。但是,也有例外。我们还发现了三个共有的人类/侏儒黑猩猩多态性,均涉及CpG二核苷酸-核苷酸,和两个共有的人类/大猩猩多态性,其中一个涉及CpG二核苷酸。我们证明基于微阵列的分析方法可以对跨足和跨足的遗传变异进行快速的比较序列分析。

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