Mapping crossover events of mouse meiotic recombination by restriction fragment ligation-based Refresh-seq

IF 13 1区 生物学 Q1 CELL BIOLOGY Cell Discovery Pub Date : 2024-03-05 DOI:10.1038/s41421-023-00638-9
Yan Wang, Yijun Chen, Junpeng Gao, Haoling Xie, Yuqing Guo, Jingwei Yang, Jun’e Liu, Zonggui Chen, Qingqing Li, Mengyao Li, Jie Ren, Lu Wen, Fuchou Tang
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Abstract

Single-cell whole-genome sequencing methods have undergone great improvements over the past decade. However, allele dropout, which means the inability to detect both alleles simultaneously in an individual diploid cell, largely restricts the application of these methods particularly for medical applications. Here, we develop a new single-cell whole-genome sequencing method based on third-generation sequencing (TGS) platform named Refresh-seq (restriction fragment ligation-based genome amplification and TGS). It is based on restriction endonuclease cutting and ligation strategy in which two alleles in an individual cell can be cut into equal fragments and tend to be amplified simultaneously. As a new single-cell long-read genome sequencing method, Refresh-seq features much lower allele dropout rate compared with SMOOTH-seq. Furthermore, we apply Refresh-seq to 688 sperm cells and 272 female haploid cells (secondary polar bodies and parthenogenetic oocytes) from F1 hybrid mice. We acquire high-resolution genetic map of mouse meiosis recombination at low sequencing depth and reveal the sexual dimorphism in meiotic crossovers. We also phase the structure variations (deletions and insertions) in sperm cells and female haploid cells with high precision. Refresh-seq shows great performance in screening aneuploid sperm cells and oocytes due to the low allele dropout rate and has great potential for medical applications such as preimplantation genetic diagnosis.

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通过基于限制性片段连接的 Refresh-seq 技术绘制小鼠减数分裂重组的交叉事件图谱
过去十年来,单细胞全基因组测序方法有了很大改进。然而,等位基因丢失(即无法同时检测单个二倍体细胞中的两个等位基因)在很大程度上限制了这些方法的应用,尤其是在医学应用方面。在此,我们开发了一种基于第三代测序(TGS)平台的新型单细胞全基因组测序方法,命名为 Refresh-seq(基于限制性片段连接的基因组扩增和 TGS)。该方法基于限制性内切酶切割和连接策略,可将单个细胞中的两个等位基因切割成相等的片段,并倾向于同时扩增。作为一种新的单细胞长线程基因组测序方法,Refresh-seq 的等位基因丢失率比 SMOOTH-seq 低得多。此外,我们还将 Refresh-seq 应用于 F1 杂交小鼠的 688 个精子细胞和 272 个雌性单倍体细胞(次级极体和孤雌生殖卵母细胞)。我们以较低的测序深度获得了小鼠减数分裂重组的高分辨率遗传图谱,并揭示了减数分裂交叉的性双态性。我们还对精子细胞和雌性单倍体细胞的结构变异(缺失和插入)进行了高精度分期。由于等位基因丢失率低,Refresh-seq 在筛选非整倍体精子细胞和卵母细胞方面表现出色,在植入前基因诊断等医学应用方面具有巨大潜力。
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来源期刊
Cell Discovery
Cell Discovery Biochemistry, Genetics and Molecular Biology-Molecular Biology
CiteScore
24.20
自引率
0.60%
发文量
120
审稿时长
20 weeks
期刊介绍: Cell Discovery is a cutting-edge, open access journal published by Springer Nature in collaboration with the Center for Excellence in Molecular Cell Science, Chinese Academy of Sciences (CAS). Our aim is to provide a dynamic and accessible platform for scientists to showcase their exceptional original research. Cell Discovery covers a wide range of topics within the fields of molecular and cell biology. We eagerly publish results of great significance and that are of broad interest to the scientific community. With an international authorship and a focus on basic life sciences, our journal is a valued member of Springer Nature's prestigious Molecular Cell Biology journals. In summary, Cell Discovery offers a fresh approach to scholarly publishing, enabling scientists from around the world to share their exceptional findings in molecular and cell biology.
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