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Differential long noncoding RNA and messenger RNA expression profiling and functional network analysis in stroke-induced neurogenesis

机译:中风诱导神经发生中的差异性长非编码RNA和信使RNA表达谱和功能网络分析。

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Background and Purpose-Adult neurogenesis contributes to neurological recovery after stroke. Long non-coding RNAs (lncRNAs) play an important role in the self-renewal and differentiation of stem cells. However, knowledge of the lncRNAs in stroke-induced neurogenesis remains unclear. Methods and Results- In the study, we isolated adult neural stem cells (NSCs) from the subventricular zone (SVZ) neurogenic region of adult non-ischemic and ischemic rats subjected to 7 day middle cerebral artery occlusion and then performed lncRNA profile analysis. In total, 155 lncRNAs were found to be significantly differentially down-regulated, while 86 lncRNAs were significantly up-regulated after stroke. Also, we identified 409 mRNAs were significantly up-regulated and 255 were down-regulated in ischemic NSCs compared with non-ischemic NSCs. We found that 4 significantly upregulated lncRNAs and 2 downregulated lncRNAs were positively correlated with their neighboring coding genes. Furthermore, the network analysis revealed matched lncRNA-mRNA correlations. A gene set enrichment analysis (GSEA) showed that Gene ontology (GO) of targeted genes that were positively modulated by lncRNAs was mainly related to synapse plasticity, cognition, neuron development, mitochondria, neurotransmitter signaling, calcium channel regulation, etc. Meanwhile, co-expressed genes negatively regulated by lncRNAs were correlated with DNA replication, cytokine production, cell adhesion, NF-κB signaling, T cell process, metabolic process, etc. Conclusions- The present study provides a comprehensive catalog of lncRNAs involved in the ischemic NSCs and provides new insight into understanding the role of lncRNAs in stroke-induced neurogenesis.
机译:背景和目的 - 成人神经发生有助于中风后神经恢复。长期非编码RNA(LNCRNA)在干细胞的自我更新和分化中起重要作用。然而,知识中风诱导的神经发生中的LNCRNA仍然尚不清楚。方法和结果 - 在研究中,来自成人非缺血性和缺血性大鼠的子宫内部区域(SVZ)神经发生区域的成人神经干细胞(NSCs)进行7天中间脑动脉闭塞,然后进行了LNCRNA谱分析。总共发现155个LNCRNA被显着差异下调,而中风后86个LNCRNA显着上调。此外,我们确定了409例MRNA显着上调,与非缺血性NSCs相比,缺血性NSC的255例下调。我们发现4个显着上调的LNCRNA和2下调的LNCRNA与相邻编码基因正相关。此外,网络分析显示出匹配的LNCRNA-mRNA相关性。一种基因设定的富集分析(GSEA)表明,LNCRNA阳性调节的靶向基因的基因本体论(GO)主要与突触可塑性,认知,神经元发育,线粒体,神经递质信号传导,钙通道调节等有关。同时,有限公司-Excressed由LNCRNA负调节的基因与DNA复制,细胞因子产生,细胞粘附,NF-κB信号传导,T细胞过程,代谢过程等结论 - 本研究提供了涉及缺血性NSCs的LNCRNA的全面目录和提供新的洞察理解LNCRNA在中风诱导的神经发生中的作用。

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