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Genome-wide search for novel human uORFs and N-terminal protein extensions using ribosomal footprinting

机译:全基因组搜索使用核糖体足迹的新型人类uORF和N末端蛋白质延伸

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So far, the annotation of translation initiation sites (TISs) has been based mostly upon bioinformatics rather than experimental evidence. We adapted ribosomal footprinting to puromycin-treated cells to generate a transcriptome-wide map of TISs in a human monocytic cell line. A neural network was trained on the ribosomal footprints observed at previously annotated AUG translation initiation codons (TICs), and used for the ab initio prediction of TISs in 5062 transcripts with sufficient sequence coverage. Functional interpretation suggested 2994 novel upstream open reading frames (uORFs) in the 5′ UTR, 1406 uORFs overlapping with the coding sequence, and 546 N-terminal protein extensions. The TIS detection method was validated on the basis of previously published alternative TISs and uORFs. Among primates, TICs in newly annotated TISs were significantly more conserved than control codons, both for AUGs and nearcognate codons. The transcriptome-wide map of novel candidate TISs derived as part of the study will shed further light on the way in which human proteome diversity is influenced by alternative translation initiation and regulation.
机译:到目前为止,翻译起始位点(TIS)的注释主要基于生物信息学而非实验证据。我们使核糖体足迹适应于嘌呤霉素处理的细胞,以在人类单核细胞系中产生TIS的转录组全图。对在先前标注的AUG翻译起始密码子(TICs)处观察到的核糖体足迹进行了神经网络训练,并将其用于从头开始预测5062个转录本中的TIS具有足够的序列覆盖率。功能解释建议在5'UTR中有2994个新颖的上游开放阅读框(uORF),与编码序列重叠的1406个uORF和546个N端蛋白质延伸。 TIS检测方法已基于先前发布的替代TIS和uORF进行了验证。在灵长类动物中,无论是AUGs还是近同源密码子,新注释的TIS中的TICs均比对照密码子保守得多。作为研究的一部分而获得的新型候选TIS的转录组全图将进一步阐明人类蛋白质组多样性受替代翻译起始和调控方式的影响。

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