首页> 外文期刊>RNA >MicroRNAs 296 and 298 are imprinted and part of the GNAS/Gnas cluster and miR-296 targets IKBKE and Tmed9.
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MicroRNAs 296 and 298 are imprinted and part of the GNAS/Gnas cluster and miR-296 targets IKBKE and Tmed9.

机译:MicroRNA 296和298被印记,并且是GNAS / Gnas簇的一部分,miR-296靶向IKBKE和Tmed9。

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摘要

Genomic imprinting is the phenomenon whereby a subset of genes is differentially expressed according to parental origin. Imprinted genes tend to occur in clusters, and microRNAs are associated with the majority of well-defined clusters of imprinted genes. We show here that two microRNAs, miR-296 and miR-298, are part of the imprinted Gnas/GNAS clusters in both mice and humans. Both microRNAs show imprinted expression and are expressed from the paternally derived allele, but not the maternal allele. They arise from a long, noncoding antisense transcript, Nespas, with a promoter more than 27 kb away. Nespas had been shown previously to act in cis to regulate imprinted gene expression within the Gnas cluster. Using microarrays and luciferase assays, IKBKE, involved in many signaling pathways, and Tmed9, a protein transporter, were verified as new targets of miR-296. Thus, Nespas has two clear functions: as a cis-acting regulator within an imprinted gene cluster and as a precursor of microRNAs that modulate gene expression in trans. Furthermore, imprinted microRNAs, including miR-296 and miR-298, impose a parental specific modulation of gene expression of their target genes.
机译:基因组印迹是一种现象,其中基因的一个子集根据亲本起源差异表达。印迹基因倾向于以簇的形式出现,并且microRNA与印迹基因的大多数定义良好的簇相关。我们在这里显示了两个microRNA,即miR-296和miR-298,是小鼠和人类中印记的Gnas / GNAS簇的一部分。两种microRNA均显示印迹的表达,并从父本衍生的等位基因表达,而不是母本等位基因表达。它们来自长的非编码反义转录物Nespas,其启动子超过27 kb。 Nespas先前已被证明可以顺式作用来调节Gnas簇内的印迹基因表达。使用微阵列和荧光素酶测定法,已证实参与许多信号传导途径的IKBKE和蛋白质转运蛋白Tmed9是miR-296的新靶标。因此,Nespas具有两个明确的功能:作为印迹基因簇内的顺式作用调节剂,以及作为反式调节基因表达的microRNA的前体。此外,包括miR-296和miR-298在内的印迹microRNA对其目标基因的基因表达施加父母特异性调节。

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