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人类多能干细胞中 DNA 复制时间的遗传结构。

The genetic architecture of DNA replication timing in human pluripotent stem cells.

机构信息

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

Department of Pediatrics, Columbia University, New York, NY, 10032, USA.

出版信息

Nat Commun. 2021 Nov 19;12(1):6746. doi: 10.1038/s41467-021-27115-9.

Abstract

DNA replication follows a strict spatiotemporal program that intersects with chromatin structure but has a poorly understood genetic basis. To systematically identify genetic regulators of replication timing, we exploited inter-individual variation in human pluripotent stem cells from 349 individuals. We show that the human genome's replication program is broadly encoded in DNA and identify 1,617 cis-acting replication timing quantitative trait loci (rtQTLs) - sequence determinants of replication initiation. rtQTLs function individually, or in combinations of proximal and distal regulators, and are enriched at sites of histone H3 trimethylation of lysines 4, 9, and 36 together with histone hyperacetylation. H3 trimethylation marks are individually repressive yet synergistically associate with early replication. We identify pluripotency-related transcription factors and boundary elements as positive and negative regulators of replication timing, respectively. Taken together, human replication timing is controlled by a multi-layered mechanism with dozens of effectors working combinatorially and following principles analogous to transcription regulation.

摘要

DNA 复制遵循严格的时空程序,与染色质结构相交织,但遗传基础知之甚少。为了系统地鉴定复制时间的遗传调控因子,我们利用了来自 349 个人的人类多能干细胞的个体间变异。我们表明,人类基因组的复制程序广泛地编码在 DNA 中,并鉴定出 1617 个顺式作用复制时间数量性状基因座(rtQTL)-复制起始的序列决定因素。rtQTL 单独起作用,或在近端和远端调节剂的组合中起作用,并且在与组蛋白 H3 赖氨酸 4、9 和 36 三甲基化以及组蛋白超乙酰化一起的组蛋白 H3 修饰位点处富集。H3 三甲基化标记单独具有抑制性,但协同与早期复制相关联。我们确定多能性相关转录因子和边界元件分别为复制时间的正和负调节剂。总之,人类复制时间受多层次机制控制,数十个效应物以组合的方式协同作用,并遵循类似于转录调控的原则。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f056/8604924/f653979da7b0/41467_2021_27115_Fig1_HTML.jpg

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