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Mathematical modeling identifies potential gene structure determinants of co-transcriptional control of alternative pre-mRNA splicing

机译:数学建模鉴定替代前mRNA剪接共转录控制的潜在基因结构决定因素

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摘要

The spliceosome catalyzes the removal of introns from pre-messenger RNA (mRNA) and subsequent pairing of exons with remarkable fidelity. Some exons are known to be skipped or included in the mature mRNA in a cell type- or context-dependent manner (cassette exons), thereby contributing to the diversification of the human proteome. Interestingly, splicing is initiated (and sometimes completed) co-transcriptionally. Here, we develop a kinetic mathematical modeling framework to investigate alternative co-transcriptional splicing (CTS) and, specifically, the control of cassette exons' inclusion. We show that when splicing is co-transcriptional, default splice patterns of exon inclusion are more likely than when splicing is post-transcriptional, and that certain exons are more likely to be regulatable (i.e. cassette exons) than others, based on the exon-intron structure context. For such regulatable exons, transcriptional elongation rates may affect splicing outcomes. Within the CTS paradigm, we examine previously described hypotheses of co-operativity between splice sites of short introns (i.e. 'intron definition') or across short exons (i.e. 'exon definition'), and find that models encoding these faithfully recapitulate observations in the fly and human genomes, respectively.
机译:缩写剂催化从信使RNA(mRNA)的除去内含子,随后与显着保真度的外显子配对。已知一些外显子以细胞类型或上下文依赖性方式(盒式外显子)跳过或包括在成熟mRNA中,从而有助于人蛋白质组的多样化。有趣的是,拼接(有时完成)联合转录。在这里,我们开发动力学数学建模框架,以研究替代的共转录剪接(CTS),具体地,控制盒式外显子的夹杂物。我们表明,当拼接是共转录时,外显子夹杂物的默认接头模式比剪接术后转录时更容易,并且某些外显子更可能是可调节的(即盒式外显子),基于外部内含子结构背景。对于这种可调节的外显子,转录伸长率可能会影响剪接结果。在CTS范例中,我们检查了短内含子(即'内含子定义')或短外显子(即'EXON定义')之间的剪接位点之间的共同操作性的假设,并发现编码这些忠实地概括的模型飞行和人类基因组。

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