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首页> 外文期刊>Journal of cellular biochemistry. >Histone Modifications Pattern Associated With a State of Mesenchymal Stem Cell Cultures Derived From Amniotic Fluid of Normal and Fetus‐Affected Gestations
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Histone Modifications Pattern Associated With a State of Mesenchymal Stem Cell Cultures Derived From Amniotic Fluid of Normal and Fetus‐Affected Gestations

机译:组蛋白修饰与衍生自正常和胎儿影响妊娠的羊水的间充质干细胞培养物相关的模式

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ABSTRACT Human amniotic fluid (AF)‐derived mesenchymal stem cells (MSCs) sharing embryonic and adult stem cells characteristics are interesting by their multipotency and the usage for regenerative medicine. However, the usefulness of these cells for revealing the fetal diseases still needs to be assessed. Here, we have analyzed the epigenetic environment in terms of histone modifications in cultures of MSCs derived from AF of normal pregnancies and those with fetal abnormalities. The comparison of MSCs samples from AF of normal pregnancies (N) and fetus‐affected (P) revealed two distinct cultures by their proliferation potential (P I and P II). Cell populations from N and P I samples had similar growth characteristics and exhibited quite similar cell surface (CD44, CD90, CD105) and stemness markers (Oct4, Nanog, Sox2, Rex1) profile that was distinct in slower growing and faster senescent P II cultures. Those differences were associated with changes in 5‐Cyt DNA methylation and alterations in the expression levels of chromatin modifiers (DNMT1, HDAC1/2), activating (H4ac, H3K4me3), and repressive (H3K9me2/me3, H3K27me3) histone marks. MSCs isolated from AF with the genetic or multifactorial fetal diseases (P II samples) were enriched with repressive histone marks and H4K16ac, H3K9ac, H3K14ac modifications. This study indicates that differential epigenetic environment reflects a state of AF‐MSCs dependently on their growth, phenotype, and stemness characteristics suggesting a way for better understanding of epigenetic regulatory mechanisms in AF‐MSCs cultures in normal and diseased gestation conditions. J. Cell. Biochem. 118: 3744–3755, 2017. ? 2017 Wiley Periodicals, Inc.
机译:摘要摘要人羊水(AF)的间充质干细胞(MSCs)共用胚胎和成体干细胞特征是通过其多能力和再生医学的使用情况感兴趣。然而,需要评估这些细胞的有用性露出胎儿疾病。在这里,我们在衍生自常规妊娠的AFS和胎儿异常的MSCs培养物中分析了表观遗传环境。 MSCS样品从AF的正常妊娠(N)和胎儿影响(P)的比较揭示了它们的增殖电位(P I和P II)的两个不同的培养。来自N和P I样品的细胞群具有相似的生长特性,并且表现出相似的细胞表面(CD44,CD90,CD105)和茎标记物(OCT4,纳米,SOX2,REX1)轮廓,其在较慢的生长和衰老的衰老P II培养物中明显。这些差异与染色质调味剂(DNMT1,HDAC1 / 2),活化(H4Ac,H3K4ME3)和压抑(H3K9ME2 / ME3,H3K27ME3)组蛋白标记的组蛋白标记的组蛋白标记有关的5-Cyt DNA甲基化和改变的差异。与遗传或多术胎儿疾病(P II样品)分离的MSCs富含抑制组蛋白标记和H4K16AC,H3K9AC,H3K14AC修饰。本研究表明,差异表观遗传环境依赖于其生长,表型和茎秆特征反映了AF-MSC的状态,这表明一种更好地理解正常和患病妊娠条件下的AF-MSCs培养物中的表观遗传调控机制。 J.Cell。生物学习。 118:3744-3755,2017 2017年Wiley期刊,Inc。

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