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Genomic Imprinting of Dopa decarboxylase in Heart and Reciprocal Allelic Expression with Neighboring Grb10

机译:多巴脱羧酶在心脏中的基因组印迹和与邻近的Grb10等位基因的相互表达

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By combining a tissue-specific microarray screen with mouse uniparental duplications, we have identified a novel imprinted gene, Dopa decarboxylase (Ddc), on chromosome 11. Ddc_exon1a is a 2-kb transcript variant that initiates from an alternative first exon in intron 1 of the canonical Ddc transcript and is paternally expressed in trabecular cardiomyocytes of the embryonic and neonatal heart. Ddc displays tight conserved linkage with the maternally expressed and methylated Grb10 gene, suggesting that these reciprocally imprinted genes may be coordinately regulated. In Dnmt3L mutant embryos that lack maternal germ line methylation imprints, we show that Ddc is overexpressed and Grb10 is silenced. Their imprinting is therefore dependent on maternal germ line methylation, but the mechanism at Ddc does not appear to involve differential methylation of the Ddc_exon1a promoter region and may instead be provided by the oocyte mark at Grb10. Our analysis of Ddc redefines the imprinted Grb10 domain on mouse proximal chromosome 11 and identifies Ddc_exon1a as the first example of a heart-specific imprinted gene.
机译:通过将组织特异性微阵列筛选与小鼠单亲重复相结合,我们在11号染色体上鉴定了一个新的印迹基因 Dopa脱羧酶(Ddc )。 Ddc_exon1a 是一个2- kb转录物变体,从典型的 Ddc 转录物的内含子1中的另一个第一外显子开始,并在胚胎和新生儿心脏的小梁型心肌细胞中父本表达。 Ddc 与母本表达和甲基化的 Grb10 基因显示出紧密的保守联系,表明这些相互印记的基因可能受到协调调控。在缺少母系生殖甲基化印记的 Dnmt3L 突变胚胎中,我们表明 Ddc 过表达,而 Grb10 被沉默。因此,它们的印记取决于母体生殖系的甲基化,但是 Ddc 的机制似乎不涉及 Ddc_exon1a 启动子区域的甲基化差异,而可能由卵母细胞提供在 Grb10 处标记。我们对 Ddc 的分析重新定义了小鼠近端11号染色体上的印迹 Grb10 域,并将 Ddc_exon1a 识别为心脏特异性印迹基因的第一个例子。

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