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Integrative transcriptome sequencing reveals extensive alternative trans-splicing and cis-backsplicing in human cells

机译:整合转录组测序揭示了人类细胞中广泛的选择性反式剪接和顺式剪接

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摘要

Transcriptionally non-co-linear (NCL) transcripts can originate from trans-splicing (trans-spliced RNA; ‘tsRNA’) or cis-backsplicing (circular RNA; ‘circRNA’). While numerous circRNAs have been detected in various species, tsRNAs remain largely uninvestigated. Here, we utilize integrative transcriptome sequencing of poly(A)- and non-poly(A)-selected RNA-seq data from diverse human cell lines to distinguish between tsRNAs and circRNAs. We identified 24,498 NCL events and found that a considerable proportion (20–35%) of them arise from both tsRNAs and circRNAs, representing extensive alternative trans-splicing and cis-backsplicing in human cells. We show that sequence generalities of exon circularization are also observed in tsRNAs. Recapitulation of NCL RNAs further shows that inverted Alu repeats can simultaneously promote the formation of tsRNAs and circRNAs. However, tsRNAs and circRNAs exhibit quite different, or even opposite, expression patterns, in terms of correlation with the expression of their co-linear counterparts, expression breadth/abundance, transcript stability, and subcellular localization preference. These results indicate that tsRNAs and circRNAs may play different regulatory roles and analysis of NCL events should take the joint effects of different NCL-splicing types and joint effects of multiple NCL events into consideration. This study describes the first transcriptome-wide analysis of trans-splicing and cis-backsplicing, expanding our understanding of the complexity of the human transcriptome.
机译:转录上的非共线性(NCL)转录本可以源自反式剪接(trans-spliced RNA;'tsRNA')或顺式反剪接(circular RNA;'circRNA')。尽管已在各种物种中检测到许多circRNA,但tsRNA仍未进行大量研究。在这里,我们利用来自不同人类细胞系的poly(A)和非poly(A)选择的RNA-seq数据的整合转录组测序来区分tsRNA和circRNA。我们鉴定了24,498个NCL事件,发现其中相当一部分(20–35%)来自tsRNA和circRNA,这代表了人类细胞中广泛的交替反式剪接和顺式剪接。我们表明,在tsRNAs中也观察到外显子环化的序列一般性。 NCL RNA的概括进一步表明,反向的Alu重复序列可以同时促进tsRNA和circRNA的形成。但是,tsRNA和circRNA在与其共线对应物的表达,表达广度/丰度,转录本稳定性和亚细胞定位偏好的相关性方面表现出完全不同甚至相反的表达模式。这些结果表明,tsRNA和circRNA可能发挥不同的调节作用,对NCL事件的分析应考虑不同NCL剪接类型的联合效应和多个NCL事件的联合效应。这项研究描述了第一个转录组范围内的反式剪接和顺式反剪接分析,扩大了我们对人类转录组复杂性的理解。

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