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活细胞中单个基因的转录依赖性迁移和全基因组运动。

Transcription-dependent mobility of single genes and genome-wide motions in live human cells.

机构信息

Center for Soft Matter Research, Department of Physics, New York University, New York, NY, 10003, USA.

出版信息

Nat Commun. 2024 Oct 22;15(1):8879. doi: 10.1038/s41467-024-51149-4.

Abstract

The human genome is highly dynamic across all scales. At the gene level, chromatin is persistently remodeled and rearranged during active processes such as transcription, replication and DNA repair. At the genome level, chromatin moves in micron-scale domains that break up and re-form over seconds, but the origin of these coherent motions is unknown. Here, we investigate the connection between genomic motions and gene-level activity. Simultaneous mapping of single-gene and genome-wide motions shows that the coupling of gene transcriptional activity to flows of the nearby genome is modulated by chromatin compaction. A motion correlation analysis suggests that a single active gene drives larger-scale motions in low-compaction regions, but high-compaction chromatin drives gene motion regardless of its activity state. By revealing unexpected connections among gene activity, spatial heterogeneities of chromatin and its emergent genome-wide motions, these findings uncover aspects of the genome's spatiotemporal organization that directly impact gene regulation and expression.

摘要

人类基因组在所有尺度上都具有高度动态性。在基因水平上,染色质在转录、复制和 DNA 修复等活跃过程中不断重塑和重排。在基因组水平上,染色质在微米尺度的域中移动,这些域在数秒内分裂和重新形成,但这些连贯运动的起源尚不清楚。在这里,我们研究了基因组运动和基因水平活动之间的联系。单基因和全基因组运动的同时映射表明,基因转录活性与附近基因组流动的耦合受染色质紧缩的调节。运动相关分析表明,单个活跃基因驱动低压缩区域的更大尺度运动,但高压缩染色质驱动基因运动,而不管其活性状态如何。通过揭示基因活性、染色质空间异质性及其新兴的全基因组运动之间的意外联系,这些发现揭示了基因组时空组织的各个方面,这些方面直接影响基因调控和表达。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9fa/11496510/1ef79a059893/41467_2024_51149_Fig1_HTML.jpg

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