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Centromeric Satellite DNAs: Hidden Sequence Variation in the Human Population

机译:着丝粒卫星DNA:人类人口中的隐藏序列变异。

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摘要

The central goal of medical genomics is to understand the inherited basis of sequence variation that underlies human physiology, evolution, and disease. Functional association studies currently ignore millions of bases that span each centromeric region and acrocentric short arm. These regions are enriched in long arrays of tandem repeats, or satellite DNAs, that are known to vary extensively in copy number and repeat structure in the human population. Satellite sequence variation in the human genome is often so large that it is detected cytogenetically, yet due to the lack of a reference assembly and informatics tools to measure this variability, contemporary high-resolution disease association studies are unable to detect causal variants in these regions. Nevertheless, recently uncovered associations between satellite DNA variation and human disease support that these regions present a substantial and biologically important fraction of human sequence variation. Therefore, there is a pressing and unmet need to detect and incorporate this uncharacterized sequence variation into broad studies of human evolution and medical genomics. Here I discuss the current knowledge of satellite DNA variation in the human genome, focusing on centromeric satellites and their potential implications for disease.
机译:医学基因组学的主要目标是了解人类生理,进化和疾病所依据的序列变异的遗传基础。功能关联研究目前忽略了跨越每个着丝粒区域和近端短臂的数百万个碱基。这些区域富含长串的串联重复序列或卫星DNA,这些序列在人类中的拷贝数和重复序列结构差异很大。人类基因组中的卫星序列变异通常如此之大,以至于可以通过细胞遗传学方法检测到,但是由于缺乏用于测量变异性的参考装配和信息学工具,当代的高分辨率疾病关联研究无法检测到这些区域的因果变异。然而,最近发现的卫星DNA变异与人类疾病之间的关联支持这些区域呈现了人类序列变异的重要且生物学重要的组成部分。因此,迫切且未满足的需求来检测并将这种未表征的序列变异并入人类进化和医学基因组学的广泛研究中。在这里,我将讨论人类基因组中卫星DNA变异的最新知识,重点是着丝粒卫星及其对疾病的潜在影响。

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