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Revealing stable processing products from ribosome-associated small RNAs by deep-sequencing data analysis

机译:通过深度测序数据分析从核糖体相关的小RNA中揭示稳定的加工产物

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摘要

The exploration of the non-protein-coding RNA (ncRNA) transcriptome is currently focused on profiling of microRNA expression and detection of novel ncRNA transcription units. However, recent studies suggest that RNA processing can be a multi-layer process leading to the generation of ncRNAs of diverse functions from a single primary transcript. Up to date no methodology has been presented to distinguish stable functional RNA species from rapidly degraded side products of nucleases. Thus the correct assessment of widespread RNA processing events is one of the major obstacles in transcriptome research. Here, we present a novel automated computational pipeline, named APART, providing a complete workflow for the reliable detection of RNA processing products from next-generation-sequencing data. The major features include efficient handling of non-unique reads, detection of novel stable ncRNA transcripts and processing products and annotation of known transcripts based on multiple sources of information. To disclose the potential of APART, we have analyzed a cDNA library derived from small ribosome-associated RNAs in Saccharomyces cerevisiae. By employing the APART pipeline, we were able to detect and confirm by independent experimental methods multiple novel stable RNA molecules differentially processed from well known ncRNAs, like rRNAs, tRNAs or snoRNAs, in a stress-dependent manner.
机译:目前,非蛋白质编码RNA(ncRNA)转录组的探索集中在microRNA表达谱分析和新型ncRNA转录单位的检测上。但是,最近的研究表明,RNA加工可能是一个多层过程,导致从单个初级转录本生成具有多种功能的ncRNA。迄今为止,还没有方法可以将稳定的功能性RNA物种与核酸酶的快速降解副产物区分开。因此,正确评估广泛的RNA加工事件是转录组研究的主要障碍之一。在这里,我们介绍了一种新颖的自动计算管道,名为APART,为从下一代测序数据中可靠地检测RNA处理产品提供了完整的工作流程。主要功能包括有效处理非唯一读取,检测新型稳定的ncRNA转录本和加工产品以及基于多种信息源注释已知的转录本。为了揭示APART的潜力,我们分析了一个来自酿酒酵母中小核糖体相关RNA的cDNA文库。通过使用APART管道,我们能够通过独立的实验方法以压力依赖的方式检测和确认从众所周知的ncRNA(如rRNA,tRNA或snoRNA)差异处理的多个新型稳定RNA分子。

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