Coming of age: ten years of next-generation sequencing technologies

生物 基因组 DNA测序 计算生物学 人类基因组 序列(生物学) 遗传学 全基因组测序 进化生物学 DNA 基因
作者
Sara Goodwin,John D. McPherson,W. Richard McCombie
出处
期刊:Nature Reviews Genetics [Nature Portfolio]
卷期号:17 (6): 333-351 被引量:4400
标识
DOI:10.1038/nrg.2016.49
摘要

Advances in DNA sequencing technologies have led to vast increases in the diversity of sequencing-based applications and in the amount of data generated. This Review discusses the current state-of-the-art technologies in both short-read and long-read DNA sequencing, their underlying mechanisms, relative strengths and limitations, and emerging applications. Since the completion of the human genome project in 2003, extraordinary progress has been made in genome sequencing technologies, which has led to a decreased cost per megabase and an increase in the number and diversity of sequenced genomes. An astonishing complexity of genome architecture has been revealed, bringing these sequencing technologies to even greater advancements. Some approaches maximize the number of bases sequenced in the least amount of time, generating a wealth of data that can be used to understand increasingly complex phenotypes. Alternatively, other approaches now aim to sequence longer contiguous pieces of DNA, which are essential for resolving structurally complex regions. These and other strategies are providing researchers and clinicians a variety of tools to probe genomes in greater depth, leading to an enhanced understanding of how genome sequence variants underlie phenotype and disease.
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