Long‐read sequencing for molecular diagnostics in constitutional genetic disorders

生物 纳米孔测序 DNA测序 计算生物学 分子诊断学 论证(复杂分析) 计算机科学 数据科学 遗传学 DNA 生物化学
作者
Laura K. Conlin,Erfan Aref‐Eshghi,Deborah McEldrew,Minjie Luo,Ramakrishnan Rajagopalan
出处
期刊:Human Mutation [Wiley]
卷期号:43 (11): 1531-1544 被引量:61
标识
DOI:10.1002/humu.24465
摘要

Long-read sequencing (LRS) has been around for more than a decade, but widespread adoption of the technology has been slow due to the perceived high error rates and high sequencing cost. This is changing due to the recent advancements to produce highly accurate sequences and the reducing costs. LRS promises significant improvement over short read sequencing in four major areas: (1) better detection of structural variation (2) better resolution of highly repetitive or nonunique regions (3) accurate long-range haplotype phasing and (4) the detection of base modifications natively from the sequencing data. Several successful applications of LRS have demonstrated its ability to resolve molecular diagnoses where short-read sequencing fails to identify a cause. However, the argument for increased diagnostic yield from LRS remains to be validated. Larger cohort studies may be required to establish the realistic boundaries of LRS's clinical utility and analytical validity, as well as the development of standards for clinical applications. We discuss the limitations of the current standard of care, and contrast with the applications and advantages of two major LRS platforms, PacBio and Oxford Nanopore, for molecular diagnostics of constitutional disorders, and present a critical argument about the potential of LRS in diagnostic settings.
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