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The fine-scale and complex architecture of human copy-number variation.

机译:人类拷贝数变异的精细和复杂的体系结构。

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摘要

Despite considerable excitement over the potential functional significance of copy-number variants (CNVs), we still lack knowledge of the fine-scale architecture of the large majority of CNV regions in the human genome. In this study, we used a high-resolution array-based comparative genomic hybridization (aCGH) platform that targeted known CNV regions of the human genome at approximately 1 kb resolution to interrogate the genomic DNAs of 30 individuals from four HapMap populations. Our results revealed that 1020 of 1153 CNV loci (88%) were actually smaller in size than what is recorded in the Database of Genomic Variants based on previously published studies. A reduction in size of more than 50% was observed for 876 CNV regions (76%). We conclude that the total genomic content of currently known common human CNVs is likely smaller than previously thought. In addition, approximately 8% of the CNV regions observed in multiple individuals exhibited genomic architectural complexity in the form of smaller CNVs within larger ones and CNVs with interindividual variation in breakpoints. Future association studies that aim to capture the potential influences of CNVs on disease phenotypes will need to consider how to best ascertain this previously uncharacterized complexity.
机译:尽管对拷贝数变异体(CNV)的潜在功能意义感到十分兴奋,但我们仍然缺乏对人类基因组中大多数CNV区域的精细结构的了解。在这项研究中,我们使用了基于高分辨率阵列的比较基因组杂交(aCGH)平台,该平台以大约1 kb的分辨率靶向人类基因组的已知CNV区,以询问来自四个HapMap种群的30个个体的基因组DNA。我们的研究结果表明,在1153个CNV基因座中,有1020个(88%)的大小实际上小于基于先前发表的研究的基因组变异数据库中记录的大小。对于876个CNV地区(76%),观察到尺寸减小了50%以上。我们得出结论,当前已知的普通人类CNV的总基因组含量可能比以前认为的要小。此外,在多个个体中观察到的大约8%的CNV区域以较小的CNV在较大的CNV和断点间存在个体差异的形式表现出基因组结构复杂性。旨在捕获CNV对疾病表型的潜在影响的未来关联研究将需要考虑如何最好地确定这种以前无法表征的复杂性。

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