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Precise annotation of human, chimpanzee, rhesus macaque and mouse mitochondrial genomes leads to insight into mitochondrial transcription in mammals

机译:精确注释人,黑猩猩,恒河猕猴和小鼠线粒体基因组导致静脉内的线粒体转录

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In the present study, we applied our 'precise annotation' to the mitochondrial (mt) genomes of human, chimpanzee, rhesus macaque and mouse using 5 ' and 3 ' end small RNAs. Our new annotations updated previous annotations. In particular, our new annotations led to two important novel findings: (1) the identification of five Conserved Sequence Blocks (CSB1, CSB2, CSB3, LSP and HSP) in the control regions; and (2) the annotation of Transcription Initiation and novel Transcription Termination Sites. Based on these annotations, we proposed a novel model of mt transcription which can account for the mt transcription and its regulation in mammals. According to our model, Transcription Termination Sites function as switches to regulate the production of short, long primary transcripts and uninterrupted transcription, rather than simply terminate the mt transcription. Moreover, the expression levels of mitochondrial transcription termination factors control the proportions of rRNAs, mRNAs and lncRNAs in total mt RNA. Our findings point to the existence of many other, as yet unidentified, Transcription Termination Sites in mammals.
机译:在本研究中,我们将我们的“精确注释”应用于人,黑猩猩,恒河猕猴和小鼠的线粒体(MT)基因组使用5'和3'末端小RNA。我们的新注释更新了以前的注释。特别是,我们的新注释导致了两个重要的新发现:(1)控制区域中的五个保守序列块(CSB1,CSB2,CSB3,LSP和HSP)的鉴定; (2)转录起始和新型转录终止位点的注释。基于这些注释,我们提出了一种新型MT转录模型,可以考虑MT转录及其在哺乳动物中的调节。根据我们的模型,转录终止位点用作切换,以调节短,长初级转录物和不间断转录的生产,而不是简单地终止MT转录。此外,线粒体转录终止因子的表达水平控制了总Mt RNA中RRNA,MRNA和LNCRNA的比例。我们的研究结果指向哺乳动物中许多其他尚未认识到的转录终止位点。

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