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复制时间和表观基因组重排与癌症中染色体重排的性质有关。

Replication timing and epigenome remodelling are associated with the nature of chromosomal rearrangements in cancer.

机构信息

Epigenetics Laboratory, Genomics and Epigenetics Division, Garvan Institute of Medical Research, Sydney, 2010, NSW, Australia.

St. Vincent's Clinical School, Faculty of Medicine, UNSW Sydney, Sydney, 2010, NSW, Australia.

出版信息

Nat Commun. 2019 Jan 24;10(1):416. doi: 10.1038/s41467-019-08302-1.

Abstract

DNA replication timing is known to facilitate the establishment of the epigenome, however, the intimate connection between replication timing and changes to the genome and epigenome in cancer remain largely uncharacterised. Here, we perform Repli-Seq and integrated epigenome analyses and demonstrate that genomic regions that undergo long-range epigenetic deregulation in prostate cancer also show concordant differences in replication timing. A subset of altered replication timing domains are conserved across cancers from different tissue origins. Notably, late-replicating regions in cancer cells display a loss of DNA methylation, and a switch in heterochromatin features from H3K9me3-marked constitutive to H3K27me3-marked facultative heterochromatin. Finally, analysis of 214 prostate and 35 breast cancer genomes reveal that late-replicating regions are prone to cis and early-replication to trans chromosomal rearrangements. Together, our data suggests that the nature of chromosomal rearrangement in cancer is related to the spatial and temporal positioning and altered epigenetic states of early-replicating compared to late-replicating loci.

摘要

DNA 复制时间已知可促进表观基因组的建立,然而,在癌症中复制时间与基因组和表观基因组变化之间的密切联系在很大程度上仍未被描述。在这里,我们进行了 Repli-Seq 和综合表观基因组分析,证明在前列腺癌中经历长程表观遗传失调的基因组区域也表现出复制时间的一致性差异。改变的复制时间域的一部分在来自不同组织来源的癌症中是保守的。值得注意的是,癌细胞中晚期复制区域显示出 DNA 甲基化的丧失,并且异染色质特征从 H3K9me3 标记的组成型转变为 H3K27me3 标记的兼性异染色质。最后,对 214 个前列腺癌和 35 个乳腺癌基因组的分析表明,晚期复制区域易发生顺式和早期复制的染色体易位。总之,我们的数据表明,癌症中染色体易位的性质与早期复制相对于晚期复制的基因座的空间和时间定位以及改变的表观遗传状态有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/775e/6345877/eedb7ca3253a/41467_2019_8302_Fig1_HTML.jpg

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