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Human Y chromosome copy number variation in the next generation sequencing era and beyond

机译:下一代测序时代及以后的人类Y染色体拷贝数变异

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摘要

Abstract The human Y chromosome provides a fertile ground for structural rearrangements owing to its haploidy and high content of repeated sequences. The methodologies used for copy number variation (CNV) studies have developed over the years. Low-throughput techniques based on direct observation of rearrangements were developed early on, and are still used, often to complement array-based or sequencing approaches which have limited power in regions with high repeat content and specifically in the presence of long, identical repeats, such as those found in human sex chromosomes. Some specific rearrangements have been investigated for decades; because of their effects on fertility, or their outstanding evolutionary features, the interest in these has not diminished. However, following the flourishing of large-scale genomics, several studies have investigated CNVs across the whole chromosome. These studies sometimes employ data generated within large genomic projects such as the DDD study or the 1000 Genomes Project, and often survey large samples of healthy individuals without any prior selection. Novel technologies based on sequencing long molecules and combinations of technologies, promise to stimulate the study of Y-CNVs in the immediate future.
机译:摘要人Y染色体由于其淘权和高含量的重复序列而为结构重排提供肥沃的地面。多年来,用于拷贝数变异(CNV)研究的方法。基于直接观察重排的低通量技术早期开发,仍然使用,经常用于补充基于阵列的或测序方法,这些方法在具有高重复含量的区域中具有有限的电力,特别是在长期相同的重复存在下,如那些在人类性染色体中发现的那些。几十年来调查了一些特定的重排;由于它们对生育能力的影响,或他们出色的进化特征,这些兴趣并没有减少。然而,在大规模基因组学的繁荣之后,几项研究已经研究了整个染色体的CNV。这些研究有时采用在大型基因组项目中产生的数据,例如DDD研究或1000个基因组项目,并且经常在没有任何先前选择的情况下调查大型健康个体样本。基于测序长分子的新技术及技术组合,承诺在立即将来刺激Y-CNV的研究。

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