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利用单分子实时测序技术探索丙型肝炎病毒基因组。

Exploring the hepatitis C virus genome using single molecule real-time sequencing.

机构信息

Department of Omics-based Medicine, Center for Preventive Medical Science, Chiba University, Chiba 260-0856, Japan.

Department of Gastroenterology and Hepatology, Graduate School of Medicine, Kyoto University, Kyoto 606-8507, Japan.

出版信息

World J Gastroenterol. 2019 Aug 28;25(32):4661-4672. doi: 10.3748/wjg.v25.i32.4661.

Abstract

Single molecular real-time (SMRT) sequencing, also called third-generation sequencing, is a novel sequencing technique capable of generating extremely long contiguous sequence reads. While conventional short-read sequencing cannot evaluate the linkage of nucleotide substitutions distant from one another, SMRT sequencing can directly demonstrate linkage of nucleotide changes over a span of more than 20 kbp, and thus can be applied to directly examine the haplotypes of viruses or bacteria whose genome structures are changing in real time. In addition, an error correction method (circular consensus sequencing) has been established and repeated sequencing of a single-molecule DNA template can result in extremely high accuracy. The advantages of long read sequencing enable accurate determination of the haplotypes of individual viral clones. SMRT sequencing has been applied in various studies of viral genomes including determination of the full-length contiguous genome sequence of hepatitis C virus (HCV), targeted deep sequencing of the HCV NS5A gene, and assessment of heterogeneity among viral populations. Recently, the emergence of multi-drug resistant HCV viruses has become a significant clinical issue and has been also demonstrated using SMRT sequencing. In this review, we introduce the novel third-generation PacBio RSII/Sequel systems, compare them with conventional next-generation sequencers, and summarize previous studies in which SMRT sequencing technology has been applied for HCV genome analysis. We also refer to another long-read sequencing platform, nanopore sequencing technology, and discuss the advantages, limitations and future perspectives in using these third-generation sequencers for HCV genome analysis.

摘要

单分子实时 (SMRT) 测序,也称为第三代测序,是一种新型的测序技术,能够生成极其长的连续序列读取。虽然传统的短读测序无法评估彼此相距较远的核苷酸替换的关联性,但 SMRT 测序可以直接显示超过 20 kbp 跨度内的核苷酸变化的关联性,因此可以直接检测其基因组结构不断变化的病毒或细菌的单倍型。此外,已经建立了一种错误纠正方法(圆形一致测序),并且对单个分子 DNA 模板的重复测序可以产生极高的准确性。长读测序的优势能够准确确定个体病毒克隆的单倍型。SMRT 测序已应用于各种病毒基因组研究中,包括丙型肝炎病毒 (HCV) 全长连续基因组序列的确定、HCV NS5A 基因的靶向深度测序以及病毒群体异质性的评估。最近,多药耐药 HCV 病毒的出现已成为一个重大的临床问题,也可以使用 SMRT 测序来证明。在这篇综述中,我们介绍了新型第三代 PacBio RSII/Sequel 系统,将其与传统的下一代测序仪进行了比较,并总结了之前应用 SMRT 测序技术进行 HCV 基因组分析的研究。我们还提到了另一种长读测序平台,纳米孔测序技术,并讨论了在 HCV 基因组分析中使用这些第三代测序仪的优点、局限性和未来展望。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e887/6718035/9c497345a1bc/WJG-25-4661-g001.jpg

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