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HRAS 转化的鼠成纤维细胞中的染色质组织和行为。

Chromatin organization and behavior in HRAS-transformed mouse fibroblasts.

机构信息

Genome Dynamics Laboratory, National Institute of Genetics, Mishima, Shizuoka, 411-8540, Japan.

Graduate Institute for Advanced Studies, SOKENDAI, Mishima, Shizuoka, 411-8540, Japan.

出版信息

Chromosoma. 2024 Apr;133(2):135-148. doi: 10.1007/s00412-024-00817-x. Epub 2024 Feb 24.

DOI:10.1007/s00412-024-00817-x
PMID:38400910
Abstract

In higher eukaryotic cells, a string of nucleosomes, where long genomic DNA is wrapped around core histones, are rather irregularly folded into a number of condensed chromatin domains, which have been revealed by super-resolution imaging and Hi-C technologies. Inside these domains, nucleosomes fluctuate and locally behave like a liquid. The behavior of chromatin may be highly related to DNA transaction activities such as transcription and repair, which are often upregulated in cancer cells. To investigate chromatin behavior in cancer cells and compare those of cancer and non-cancer cells, we focused on oncogenic-HRAS (Gly12Val)-transformed mouse fibroblasts CIRAS-3 cells and their parental 10T1/2 cells. CIRAS-3 cells are tumorigenic and highly metastatic. First, we found that HRAS-induced transformation altered not only chromosome structure, but also nuclear morphology in the cell. Using single-nucleosome imaging/tracking in live cells, we demonstrated that nucleosomes are locally more constrained in CIRAS-3 cells than in 10T1/2 cells. Consistently, heterochromatin marked with H3K27me3 was upregulated in CIRAS-3 cells. Finally, Hi-C analysis showed enriched interactions of the B-B compartment in CIRAS-3 cells, which likely represents transcriptionally inactive chromatin. Increased heterochromatin may play an important role in cell migration, as they have been reported to increase during metastasis. Our study also suggests that single-nucleosome imaging provides new insights into how local chromatin is structured in living cells.

摘要

在高等真核细胞中,核小体串,即长基因组 DNA 围绕核心组蛋白缠绕的结构,会不规则地折叠成许多浓缩的染色质结构域,这一现象已通过超分辨率成像和 Hi-C 技术得到揭示。在这些结构域内,核小体发生波动,并在局部表现得像液体一样。染色质的行为可能与 DNA 转录和修复等活性高度相关,这些活性在癌细胞中常被上调。为了研究癌细胞中的染色质行为,并比较癌细胞和非癌细胞中的染色质行为,我们重点研究了致癌基因 HRAS(甘氨酸 12 位缬氨酸取代)转化的小鼠成纤维细胞 CIRAS-3 及其亲本 10T1/2 细胞。CIRAS-3 细胞具有致瘤性和高度转移性。首先,我们发现 HRAS 诱导的转化不仅改变了染色体结构,还改变了细胞的核形态。通过对活细胞中单核小体的成像/追踪,我们证明了核小体在 CIRAS-3 细胞中的局部约束程度高于 10T1/2 细胞。一致地,CIRAS-3 细胞中 H3K27me3 标记的异染色质上调。最后,Hi-C 分析显示,CIRAS-3 细胞中 B-B 区室的相互作用增强,这可能代表转录不活跃的染色质。异染色质的增加可能在细胞迁移中起重要作用,因为它们在转移过程中被报道会增加。我们的研究还表明,单核小体成像为研究活细胞中局部染色质的结构提供了新的视角。

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本文引用的文献

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Condensed but liquid-like domain organization of active chromatin regions in living human cells.活体细胞中活性染色质区域的凝聚但类似液体的结构域组织。
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Nucleotide metabolism: a pan-cancer metabolic dependency.核苷酸代谢:一种泛癌代谢依赖性。
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Chromosome Conformation Capture for Large Genomes.大基因组的染色体构象捕获。
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Single nucleosome tracking to study chromatin plasticity.单核小体追踪研究染色质可塑性。
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Nuclear deformation guides chromatin reorganization in cardiac development and disease.核形变指导心脏发育和疾病中的染色质重排。
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