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The Murine PSE/TATA-Dependent Transcriptome: Evidence of Functional Homologies with Its Human Counterpart

机译:小鼠PSE / TATA依赖的转录组:功能同源的证据与人类的对立面。

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摘要

A series of recent studies demonstrated an unexpectedly high frequency of intronic RNA polymerase (pol) III transcription units spread throughout the human genome. The investigation of a subset of these transcripts revealed their tissue/cell-specific transcription together with the involvement in relevant physiopathological pathways. Despite this evidence, these transcripts did not seem to have murine orthologs, based on their nucleotide sequence, resulting in a limitation of the experimental approaches aimed to study their function. In this work, we have extended our investigation to the murine genome identifying 121 pairs of mouse/human transcripts displaying syntenic subchromosomal localization. The analysis in silico of this set of putative noncoding (nc)RNAs suggest their association with alternative splicing as suggested by recent experimental evidence. The investigation of one of these pairs taken as experimental model in mouse hippocampal neurons provided evidence of a human/mouse functional homology that does not depend on underlying sequence conservation. In this light, the collection of transcriptional units here reported can be considered as a novel source for the identification and the study of novel regulatory elements involved in relevant biological processes.
机译:一系列最新研究表明,内含子RNA聚合酶(pol)III转录单元意外地以高频率分布在整个人类基因组中。对这些转录子的子集的研究揭示了它们的组织/细胞特异性转录以及参与相关的生理病理学途径。尽管有这些证据,但基于其核苷酸序列,这些转录本似乎没有鼠类直向同源物,从而导致旨在研究其功能的实验方法受到限制。在这项工作中,我们将研究扩展到了鼠类基因组,以鉴定121对显示同系亚染色体定位的小鼠/人类转录本。对这套假定的非编码(nc)RNA的计算机分析表明,它们与最近的实验证据表明的可变剪接相关。在小鼠海马神经元中作为实验模型的这些对之一的研究提供了不依赖于潜在序列保守性的人/小鼠功能同源性的证据。因此,这里报道的转录单位的收集可被认为是鉴定和研究涉及相关生物学过程的新型调控元件的新来源。

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