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低复制应激引发细胞类型特异性可遗传的晚期复制定时。

Low Replicative Stress Triggers Cell-Type Specific Inheritable Advanced Replication Timing.

机构信息

Centre de Recherches en Cancérologie de Toulouse (CRCT), UMR1037 Inserm, University Paul Sabatier III, ERL5294 CNRS, 2 Avenue Hubert Curien, 31037 Toulouse, France.

Université de Paris, CNRS, Institut Jacques Monod, DNA Replication Pathologies Team, F-75006 Paris, France.

出版信息

Int J Mol Sci. 2021 May 7;22(9):4959. doi: 10.3390/ijms22094959.

Abstract

DNA replication timing (RT), reflecting the temporal order of origin activation, is known as a robust and conserved cell-type specific process. Upon low replication stress, the slowing of replication forks induces well-documented RT delays associated to genetic instability, but it can also generate RT advances that are still uncharacterized. In order to characterize these advanced initiation events, we monitored the whole genome RT from six independent human cell lines treated with low doses of aphidicolin. We report that RT advances are cell-type-specific and involve large heterochromatin domains. Importantly, we found that some major late to early RT advances can be inherited by the unstressed next-cellular generation, which is a unique process that correlates with enhanced chromatin accessibility, as well as modified replication origin landscape and gene expression in daughter cells. Collectively, this work highlights how low replication stress may impact cellular identity by RT advances events at a subset of chromosomal domains.

摘要

DNA 复制时间(RT)反映了起始激活的时间顺序,是一种稳健且保守的细胞类型特异性过程。在低复制压力下,复制叉的减缓会导致已被充分记录的 RT 延迟,与遗传不稳定性相关,但也会产生尚未被描述的 RT 提前。为了描述这些提前的起始事件,我们监测了六种独立的人细胞系在低剂量阿非迪霉素处理下的全基因组 RT。我们报告称,RT 提前是细胞类型特异性的,涉及大的异染色质区域。重要的是,我们发现一些主要的晚期到早期 RT 提前可以被未受压力的下一代细胞继承,这是一个独特的过程,与增强的染色质可及性以及子细胞中复制起始区域景观和基因表达的改变相关。总的来说,这项工作强调了低复制压力如何通过染色体区域子集的 RT 提前事件影响细胞身份。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e6a2/8125030/871efe0646e9/ijms-22-04959-g001.jpg

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