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首页> 外文期刊>Developmental biology >miR-17 family miRNAs are expressed during early mammalian development and regulate stem cell differentiation.
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miR-17 family miRNAs are expressed during early mammalian development and regulate stem cell differentiation.

机译:miR-17家族miRNA在哺乳动物早期发育中表达并调节干细胞分化。

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摘要

MicroRNAs are small non-coding RNAs that regulate protein expression by binding 3'UTRs of target mRNAs, thereby inhibiting translation. Similar to siRNAs, miRNAs are cleaved by Dicer. Mouse and ES cell Dicer mutants demonstrate that microRNAs are necessary for embryonic development and cellular differentiation. However, technical obstacles and the relative infancy of this field have resulted in few data on the functional significance of individual microRNAs. We present evidence that miR-17 family members, miR-17-5p, miR-20a, miR-93, and miR-106a, are differentially expressed in developing mouse embryos and function to control differentiation of stem cells. Specifically, miR-93 localizes to differentiating primitive endoderm and trophectoderm of the blastocyst. We also observe high miR-93 and miR-17-5p expression within the mesoderm of gastrulating embryos. Using an ES cell model system, we demonstrate that modulation of these miRNAs delays or enhances differentiation into the germ layers. Additionally, we demonstrate that these miRNAs regulate STAT3 mRNA in vitro. We suggest that STAT3, a known ES cell regulator, is one target mRNA responsible for the effects of these miRNAs on cellular differentiation.
机译:MicroRNA是小的非编码RNA,可通过结合靶mRNA的3'UTR来调节蛋白质表达,从而抑制翻译。与siRNA相似,miRNA被Dicer切割。小鼠和ES细胞Dicer突变体表明,microRNA对于胚胎发育和细胞分化是必需的。但是,该领域的技术障碍和相对起步阶段导致有关单个microRNA功能意义的数据很少。我们目前的证据表明,miR-17家族成员,miR-17-5p,miR-20a,miR-93和miR-106a在发育中的小鼠胚胎中差异表达,并具有控制干细胞分化的功能。具体而言,miR-93定位于胚泡的原始内胚层和滋养外胚层。我们还观察到胃胚胚中胚层中高miR-93和miR-17-5p表达。使用ES细胞模型系统,我们证明了对这些miRNA的调节可延迟或增强向胚层的分化。此外,我们证明了这些miRNA在体外调节STAT3 mRNA。我们建议,STAT3,一种已知的ES细胞调节剂,是负责这些miRNA对细胞分化的作用的一种靶标mRNA。

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