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首页> 外文期刊>The Journal of Reproduction and Development >Inheritance of histone H3 methylation in reprogramming of somatic nuclei following nuclear transfer.
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Inheritance of histone H3 methylation in reprogramming of somatic nuclei following nuclear transfer.

机译:核转移后体细胞核重编程中组蛋白H3甲基化的遗传。

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摘要

Successful cloning requires reprogramming of epigenetic information of the somatic nucleus to an embryonic state. However, the molecular mechanisms regarding epigenetic reprogramming of the somatic chromatin are unclear. Herein, we transferred NIH3T3 cell nuclei into enucleated mouse oocytes and evaluated the histone H3 dimethyl-lysine 4 (H3K4me2) dynamics by immunocytochemistry. A low level of H3K4me2 in the somatic chromatin was maintained in pseudo-pronuclei. Unlike in vitro fertilized (IVF) embryos, the methylation level of nuclear transfer (NT) embryos was significantly increased at the 8-cell stage. NT embryos showed lower H3K4me2 intensity than IVF embryos at the 2-cell stage, which is when the mouse embryonic genome is activated. Moreover, the H3K4me2 signal was weak in the recloned embryos derived from single blastomeres of the NT embryos, whereas it was intense in those from IVF embryos. Two imprinted genes, U2afbp-rs and Xist, were abnormally transcribed in cloned embryos compared with IVF embryos, and this was partly correlated to the H3K4me2 level. Our results suggest that abnormal reprogramming of epigenetic markers such as histone acetylation and methylation may lead to dysregulation of gene expression in cloned embryos.
机译:成功的克隆需要将体细胞核的表观遗传信息重新编程为胚胎状态。然而,尚不清楚有关体染色质的表观遗传重编程的分子机制。在这里,我们将NIH3T3细胞核转移到去核的小鼠卵母细胞中,并通过免疫细胞化学评估了组蛋白H3二甲基赖氨酸4(H3K4me2)动力学。假核中体染色质中的H3K4me2含量较低。与体外受精(IVF)胚胎不同,在8细胞阶段,核移植(NT)胚胎的甲基化水平显着提高。在2细胞阶段,这是小鼠胚胎基因组被激活时,NT胚胎显示的IV3胚胎强度低于IVF胚胎。此外,H3K4me2信号在来自NT胚胎的单个卵裂球的克隆克隆胚胎中较弱,而在IVF胚胎中则较强。与IVF胚胎相比,克隆的胚胎中有两个印迹基因U2afbp-rs和Xist异常转录,这部分与H3K4me2水平相关。我们的结果表明,表观遗传标记的异常重编程,例如组蛋白乙酰化和甲基化,可能导致克隆胚胎中基因表达的失调。

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