首页> 美国卫生研究院文献>Frontiers in Molecular Biosciences >Systematic Analysis of Gene Expression Profiles Controlled by hnRNP Q and hnRNP R Two Closely Related Human RNA Binding Proteins Implicated in mRNA Processing Mechanisms
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Systematic Analysis of Gene Expression Profiles Controlled by hnRNP Q and hnRNP R Two Closely Related Human RNA Binding Proteins Implicated in mRNA Processing Mechanisms

机译:系统分析的hnRNP Q和hnRNP R两个密切相关的人类RNA结合蛋白参与mRNA加工机制的基因表达谱的控制。

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摘要

Heteregeneous ribonucleoproteins (hnRNPs) are a family of RNA-binding proteins that take part in all processes that involve mRNA maturation. As a consequence, alterations of their homeostasis may lead to many complex pathological disorders, such as neurodegeneration and cancer. For many of these proteins, however, their exact function and cellular targets are still not very well known. Here, we focused the attention on two hnRNP family members, hnRNP Q and hnRNP R, that we previously found affecting TDP-43 activity both in Drosophila melanogaster and human neuronal cell line. Classification of these two human proteins as paralogs is suported by the high level of sequence homology and by the observation that in fly they correspond to the same protein, namely Syp. We profiled differentially expressed genes from RNA-Seq and generated functional enrichment results after silencing of hnRNP Q and hnRNP R in neuroblastoma SH-SY5Y cell line. Interestingly, despite their high sequence similarity, these two proteins were found to affect different cellular pathways, especially with regards to neurodegeneration, such as PENK, NGR3, RAB26, JAG1, as well as inflammatory response, such as TNF, ICAM1, ICAM5, and TNFRSF9. In conclusion, human hnRNP Q and hnRNP R may be considered potentially important regulators of neuronal homeostasis and their disruption could impair distinct pathways in the central nervous system axis, thus confirming the importance of their conservation during evolution.
机译:异构核糖核蛋白(hnRNPs)是一类RNA结合蛋白,参与涉及mRNA成熟的所有过程。结果,其体内稳态的改变可能导致许多复杂的病理疾病,例如神经变性和癌症。然而,对于许多这些蛋白质,其确切功能和细胞靶标仍然不是很了解。在这里,我们将注意力集中在两个hnRNP家族成员hnRNP Q和hnRNP R上,我们先前发现它们会影响果蝇和人神经元细胞系中的TDP-43活性。通过高水平的序列同源性和观察到它们在飞行中对应于相同的蛋白质即Syp,支持了将这两种人类蛋白质分类为旁系同源物。我们从神经母细胞瘤SH-SY5Y细胞系中的hnRNP Q和hnRNP R沉默后,分析了RNA-Seq差异表达的基因并产生了功能丰富的结果。有趣的是,尽管它们具有很高的序列相似性,但发现这两种蛋白会影响不同的细胞途径,尤其是在神经退行性疾病方面,例如PENK,NGR3,RAB26,JAG1,以及炎症反应,例如TNF,ICAM1,ICAM5和TNFRSF9。总之,人类hnRNP Q和hnRNP R可能被认为是神经元稳态的潜在重要调节剂,它们的破坏可能损害中枢神经系统轴的独特途径,从而证实了它们在进化过程中保守的重要性。

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