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机械应力会影响 GNAS 异构体的甲基化模式和 hAT-MSCs 的成骨分化。

Mechanical stress affects methylation pattern of GNAS isoforms and osteogenic differentiation of hAT-MSCs.

机构信息

Laboratory of Biology, Faculty of Medicine, School of Health Sciences, University of Ioannina, 45110, Greece.

Department of Biomedical Research, Institute of Molecular Biology and Biotechnology, Foundation for Research and Technology-Hellas (FORTH), Ioannina 45110, Greece; Laboratory of Biological Chemistry, Medical Faculty, School of Health Sciences, University of Ioannina, Ioannina 45110, Greece.

出版信息

Biochim Biophys Acta Mol Cell Res. 2017 Aug;1864(8):1371-1381. doi: 10.1016/j.bbamcr.2017.05.005. Epub 2017 May 5.

Abstract

Mechanical stress exerts a substantial role on skeletal-cell renewal systems, whereas accumulating evidence suggests that epigenetic mechanisms induce changes and differential gene expression. Although the underlying mechanisms remain to be fully elucidated, our study suggests that the influence of the long term mechanical stimulation elicits epigenetic modifications controlling osteogenic differentiation of human adipose tissue multipotential stromal cells (hAT-MSCs) and contributes to an accelerating in vitro osteogenesis. GNAS imprinting gene acts as a critical regulator of osteoblast differentiation and is implicated in human genetic disorders with pathological formation of ectopic-skeletal bone. Investigating a wide variety of stimuli, we showed that daily mechanical stretch on hAT-MSCs of 7th and 15th days' intervals induced a significant down-regulation in DNA methylation status of critical CpG sites of NESP and GNASXL isoforms, accompanied by up-regulation of the corresponding gene transcripts, and osteogenic differentiation earlier in culture. Importantly, methylation analysis of differentiating bone marrow-derived MSCs revealed similar methylation patterns. Bioinformatic analysis further showed that all CpG islands exhibiting significant methylation alterations encompassed transcriptional repressor CTCF binding sites. We hereby emphasize the need to investigate the epigenetic alterations on hAT-MSCs during environmental mechanical forces and to consider how the knowledge gained through these studies may foster new means of symptoms prevention and management of ectopic bone formation in the clinic.

摘要

机械应力对骨骼细胞更新系统起着重要作用,而越来越多的证据表明,表观遗传机制会诱导变化和差异基因表达。尽管潜在的机制仍有待充分阐明,但我们的研究表明,长期机械刺激的影响会引起表观遗传修饰,控制人脂肪组织多能基质细胞(hAT-MSCs)的成骨分化,并有助于加速体外成骨。GNAS 印迹基因作为成骨细胞分化的关键调节剂,与人类遗传疾病中异位骨骼形成有关。在研究了各种各样的刺激因素后,我们发现第 7 天和第 15 天对 hAT-MSCs 进行每日机械拉伸会导致关键 CpG 位点的 DNA 甲基化状态显著下调,同时相应基因转录物上调,并在培养早期促进成骨分化。重要的是,分化的骨髓间充质干细胞的甲基化分析显示出类似的甲基化模式。生物信息学分析进一步表明,所有表现出显著甲基化改变的 CpG 岛都包含转录抑制因子 CTCF 结合位点。因此,我们强调需要研究环境机械力对 hAT-MSCs 的表观遗传改变,并考虑通过这些研究获得的知识如何为临床预防和管理异位骨形成的症状提供新的手段。

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