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Mapping the Human Reference Genome’s Missing Sequence by Three-Way Admixture in Latino Genomes

机译:通过拉丁美洲基因组中的三向混合法绘制人类参考基因组的缺失序列图

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摘要

A principal obstacle to completing maps and analyses of the human genome involves the genome’s “inaccessible” regions: sequences (often euchromatic and containing genes) that are isolated from the rest of the euchromatic genome by heterochromatin and other repeat-rich sequence. We describe a way to localize these sequences by using ancestry linkage disequilibrium in populations that derive ancestry from at least three continents, as is the case for Latinos. We used this approach to map the genomic locations of almost 20 megabases of sequence unlocalized or missing from the current human genome reference (NCBI Genome GRCh37)—a substantial fraction of the human genome’s remaining unmapped sequence. We show that the genomic locations of most sequences that originated from fosmids and larger clones can be admixture mapped in this way, by using publicly available whole-genome sequence data. Genome assembly efforts and future builds of the human genome reference will be strongly informed by this localization of genes and other euchromatic sequences that are embedded within highly repetitive pericentromeric regions.
机译:完成人类基因组图谱和分析的主要障碍涉及基因组的“难以接近的”区域:通过异染色质和其他富含重复序列的序列与其他常染色体基因组隔离的序列(常为常染色体并包含基因)。我们描述了一种方法,可以通过在至少三大洲获得祖先的人口中使用祖先联系不平衡来进行定位,就像拉丁美洲人一样。我们使用这种方法来绘制当前人类基因组参考文献(NCBI Genome GRCh37)中未定位或缺失的近20兆碱基序列的基因组位置,这是人类基因组剩余的未映射序列的很大一部分。我们表明,通过使用公开可用的全基因组序列数据,可以以这种方式将来自fosmids和较大克隆的大多数序列的基因组位置进行混合定位。基因组组装的努力和人类基因组参考的未来构建将通过嵌入高度重复的着丝粒中心区域内的基因和其他常染色体序列的这种定位而获得强烈的信息。

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