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下一代测序技术实现了人类着丝粒复制时间的时空分辨率。

Next-Generation Sequencing Enables Spatiotemporal Resolution of Human Centromere Replication Timing.

机构信息

Department of Molecular Biology and Genetics, Cornell University, Ithaca, NY 14853, USA.

Weill Institute for Cell and Molecular Biology, Cornell University, Ithaca, NY 14853, USA.

出版信息

Genes (Basel). 2019 Apr 2;10(4):269. doi: 10.3390/genes10040269.

Abstract

Centromeres serve a critical function in preserving genome integrity across sequential cell divisions, by mediating symmetric chromosome segregation. The repetitive, heterochromatic nature of centromeres is thought to be inhibitory to DNA replication, but has also led to their underrepresentation in human reference genome assemblies. Consequently, centromeres have been excluded from genomic replication timing analyses, leaving their time of replication unresolved. However, the most recent human reference genome, hg38, included models of centromere sequences. To establish the experimental requirements for achieving replication timing profiles for centromeres, we sequenced G₁- and S-phase cells from five human cell lines, and aligned the sequence reads to hg38. We were able to infer DNA replication timing profiles for the centromeres in each of the five cell lines, which showed that centromere replication occurs in mid-to-late S phase. Furthermore, we found that replication timing was more variable between cell lines in the centromere regions than expected, given the distribution of variation in replication timing genome-wide. These results suggest the potential of these, and future, sequence models to enable high-resolution studies of replication in centromeres and other heterochromatic regions.

摘要

着丝粒在介导染色体的对称分离方面起着至关重要的作用,从而维持了基因组在连续细胞分裂过程中的完整性。着丝粒的重复、异染色质性质被认为对 DNA 复制具有抑制作用,但也导致了它们在人类参考基因组组装中的代表性不足。因此,着丝粒已被排除在基因组复制时间分析之外,其复制时间仍未解决。然而,最新的人类参考基因组 hg38 包含了着丝粒序列的模型。为了确定获得着丝粒复制时间图谱的实验要求,我们从五个人类细胞系中分离了 G₁ 期和 S 期细胞,并将序列读取与 hg38 进行比对。我们能够推断出五个细胞系中的每一个着丝粒的 DNA 复制时间图谱,结果表明着丝粒复制发生在 S 期的中后期。此外,我们发现,与整个基因组复制时间变异的分布相比,着丝粒区域的细胞系之间的复制时间变异更为多变。这些结果表明,这些(以及未来的)序列模型有潜力实现对着丝粒和其他异染色质区域复制的高分辨率研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3b7c/6523654/c1e027503cb2/genes-10-00269-g001.jpg

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