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Identification of miRNomes associated with adult neurogenesis after stroke using Argonaute 2-based RNA sequencing

机译:使用Argonaute 2基RNA测序识别中风后脑卒中后与成人神经发生相关的MIRNOMES

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摘要

Neurogenesis is associated with functional recovery after stroke. However, the underlying molecular mechanisms have not been fully investigated. Using an Ago2-based RNA immunoprecipitation to immunoprecipated Ago2-RNA complexes followed by RNA sequencing (Ago2 RIP-seq) approach, we profiled the miRNomes in neural progenitor cells (NPCs) harvested from the subventricular zone (SVZ) of the lateral ventricles of young adult rats. We identified more than 7 and 15million reads in normal and ischemic NPC libraries, respectively. We found that stroke substantially changed Ago2-associated miRNA profiles in NPCs compared to those in non-ischemic NPCs. We also discovered a new complex repertoire of isomiRs and multiple miRNA-miRNA* pairs and numerous novel miRNAs in the non-ischemic and ischemic NPCs. Among them, pc-3p-17172 significantly regulated NPC proliferation and neuronal differentiation. Collectively, the present study reveals profiles of Ago2-associated miRNomes in non-ischemic and ischemic NPCs, which provide a molecular basis to further investigate the role of miRNAs in mediating adult neurogenesis under physiological and ischemic conditions.
机译:神经发生与中风后功能恢复有关。然而,潜在的分子机制尚未完全研究。使用前一个基于RNA免疫沉淀到免疫折叠前2-RNA复合物,然后进行RNA测序(前rip-SEQ)方法,我们在侧向腔内(SVZ)的神经祖细胞(NPC)中分析了从侧脑室(SVZ)的神经血管血管血管成人大鼠。我们分别识别出超过7个以上的正常和缺血性NPC库读数。我们发现与非缺血NPC中的那些相比,中风基本上改变了NPC中的2-相关的miRNA谱。我们还发现了一种新的复杂的ISOMIR和多种miRNA-miRNA *对,并且在非缺血性和缺血性NPC中具有许多新的miRNA。其中,PC-3P-17172显着调节NPC增殖和神经元分化。本研究揭示了前缺血性和缺血性NPC中的2-联合的MIRNOMS的概况,其提供了分子基础,以进一步研究MiRNA在生理和缺血条件下介导成人神经发生的作用。

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