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表观遗传景观分析揭示了破骨细胞生成过程中早期染色质可及性降低的重要性。

Epigenetic landscape analysis reveals the significance of early reduced chromatin accessibility in osteoclastogenesis.

作者信息

Lee Sangyong, Kim Myoung Jun, Ahn Seor I, Choi Sung Kyung, Min Keun Young, Choi Wahn Soo, You Jueng Soo

机构信息

School of Medicine, Konkuk University, Chungju 27478, Republic of Korea.

School of Medicine, Konkuk University, Chungju 27478, Republic of Korea; KU Open Innovation Center, Research Institute of Medical Science, Konkuk University, Republic of Korea.

出版信息

Bone. 2023 Dec;177:116918. doi: 10.1016/j.bone.2023.116918. Epub 2023 Sep 20.

Abstract

Recently improved techniques could provide snapshots of chromatin structure generated based on chromatin accessibility. Since chromatin accessibility determines transcriptional potential, it has been attempted in a variety of cell systems. However, there has been no genome-wide analysis of chromatin accessibility for the entire murine osteoclast (OC) differentiation process. We performed an Assay for Transposase-Accessible Chromatin (ATAC)-sequencing (seq) during RANKL-induced OC differentiation and found that global chromatin accessibility decreased, especially early in OC differentiation. The global histone H3K27Ac level, an active histone modification mark, was diminished during OC differentiation by western blot and histone extract experiments. Its genomic enrichment was also reduced based on publicly available H3K27Ac chromatin immunoprecipitation (ChIP)-seq data. ATAC-seq and H3K27Ac ChIP-seq data demonstrated that RANKL induced a less accessible chromatin state during OC differentiation. Restoration of reduced H3K27Ac, presumably representing accessible states upon acetate treatment, suppresses OC differentiation by provoking immune-related gene expression. Subsequential integrative analysis of ATAC-seq, RNA-seq after acetate treatment, and H3K27Ac ChIP-seq reveals that Irf8 and its downstream targets are the most vulnerable to chromatin accessibility changes and acetate supplementation. Taken together, our study generated chromatin accessibility maps during the whole OC differentiation and suggested perturbation of chromatin accessibility might be a potential therapeutic strategy for excessive OC diseases.

摘要

最近改进的技术能够提供基于染色质可及性生成的染色质结构快照。由于染色质可及性决定转录潜能,因此已在多种细胞系统中进行了尝试。然而,尚未对整个小鼠破骨细胞(OC)分化过程进行全基因组范围的染色质可及性分析。我们在RANKL诱导的OC分化过程中进行了转座酶可及染色质分析(ATAC)测序,发现整体染色质可及性降低,尤其是在OC分化早期。通过蛋白质免疫印迹和组蛋白提取物实验发现,在OC分化过程中,作为一种活跃组蛋白修饰标记的整体组蛋白H3K27Ac水平降低。基于公开可用的H3K27Ac染色质免疫沉淀(ChIP)测序数据,其基因组富集也减少。ATAC测序和H3K27Ac ChIP测序数据表明,RANKL在OC分化过程中诱导了一种染色质可及性较低的状态。恢复降低的H3K27Ac(可能代表乙酸处理后的可及状态)通过引发免疫相关基因表达来抑制OC分化。对ATAC测序、乙酸处理后的RNA测序和H3K27Ac ChIP测序进行后续综合分析发现,Irf8及其下游靶点对染色质可及性变化和乙酸补充最为敏感。综上所述,我们的研究生成了整个OC分化过程中的染色质可及性图谱,并表明染色质可及性的扰动可能是治疗过度OC疾病的一种潜在策略。

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Chromatin Accessibility Predetermines Odontoblast Terminal Differentiation.染色质可及性预先决定成牙本质细胞终末分化。
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