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首页> 外文期刊>Cerebral cortex >In Vitro Corticogenesis from Embryonic Stem Cells Recapitulates the In Vivo Epigenetic Control of Imprinted Gene Expression
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In Vitro Corticogenesis from Embryonic Stem Cells Recapitulates the In Vivo Epigenetic Control of Imprinted Gene Expression

机译:来自胚胎干细胞的体外皮质生成促成了印迹基因表达的体内表观遗传控制

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In vitro corticogenesis from embryonic stem cells (ESCs) is an attractive model of cortical development and a promising tool for cortical therapy. It is unknown to which extent epigenetic mechanisms crucial for cortex development and function, such as parental genomic imprinting, are recapitulated by in vitro corticogenesis. Here, using genome-wide transcriptomic and methylation analyses on hybrid mouse tissues and cells, we find a high concordance of imprinting status between in vivo and ESC-derived cortices. Notably, in vitro corticogenesis strictly reproduced the in vivo parent-of-origin-dependent expression of 41 imprinted genes (IGs), including Mest and Cdkn1c known to control corticogenesis. Parent-of-origin-dependent DNA methylation was also conserved at 14 of 18 imprinted differentially methylated regions. The least concordant imprinted locus was Gpr1-Zdbf2, where the aberrant bi-allelic expression of Zdbf2 and Adam23 was concomitant with a gain of methylation on the maternal allele in vitro. Combined, our data argue for a broad conservation of the epigenetic mechanisms at imprinted loci in cortical cells derived from ESCs. We propose that in vitro corticogenesis helps to define the still poorly understood mechanisms that regulate imprinting in the brain and the roles of IGs in cortical development.
机译:来自胚胎干细胞的体外皮质发生(ESC)是皮质发育的有吸引力的模型和皮质治疗的有希望的工具。目前未知,通过体外皮质发生,重新携带皮质发育和诸如父母基因组印记的皮层发育和功能的表观遗传机制是至关重要的。这里,在杂交小鼠组织和细胞上使用基因组的转录组和甲基化分析,在体内和ESC衍生的皮质中发现印记状态的高度一致性。值得注意的是,体外皮质发生严格地将41个印迹基因(IGS)的依赖性依赖性表达(包括已知对控制皮质发生的最初和CDKN1C的依赖性依赖性表达。寄生原因依赖性DNA甲基化也在18个印迹差异甲基化区域中保存。最常用的印迹基因座是GPR1-ZDBF2,其中ZDBF2和Adam23的异常双等表达在体外母体等位基因的增益伴随着甲基化。结合,我们的数据争论从源自escs的皮质细胞中的印迹基因座的表观遗传机制广泛保护。我们提出体外皮质发生有助于定义调节脑中印迹的仍然较差的机制以及IGS在皮质发育中的作用。

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