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Splicing of internal large exons is defined by novel cis-acting sequence elements

机译:内部大外显子的剪接由新型顺式作用序列元件定义

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Human internal exons have an average size of 147?nt, and most are <300?nt. This small size is thought to facilitate exon definition. A small number of large internal exons have been identified and shown to be alternatively spliced. We identified 1115 internal exons >1000?nt in the human genome; these were found in 5% of all protein-coding genes, and most were expressed and translated. Surprisingly, 40% of these were expressed at levels similar to the flanking exons, suggesting they were constitutively spliced. While all of the large exons had strong splice sites, the constitutively spliced large exons had a higher ratio of splicing enhancers/silencers and were more conserved across mammals than the alternatively spliced large exons. We asked if large exons contain specific sequences that promote splicing and identified 38 sequences enriched in the large exons relative to small exons. The consensus sequence is C-rich with a central invariant CA dinucleotide. Mutation of these sequences in a candidate large exon indicated that these are important for recognition of large exons by the splicing machinery. We propose that these sequences are large exon splicing enhancers (LESEs).
机译:人体内外显子的平均大小为147nt,大多数小于300nt。这种小尺寸被认为有利于外显子的定义。少数大的内部外显子已被鉴定并显示为可剪接的。我们在人类基因组中鉴定出1115个内部外显子> 1000?nt。在所有蛋白质编码基因的5%中发现了这些蛋白,并且大多数被表达和翻译了。令人惊讶的是,其中40%的表达水平与侧翼外显子相似,表明它们是组成性剪接的。尽管所有的大外显子都有很强的剪接位点,但组成性剪接的大外显子比选择性剪接的大外显子具有更高的剪接增强子/沉默子比例,并且在哺乳动物中更保守。我们询问大外显子是否包含促进剪接的特定序列,并确定了相对于小外显子而言,在大外显子中富集的38个序列。共有序列富含C,具有中央不变的CA二核苷酸。这些序列在候选大外显子中的突变表明,这些对于通过剪接机识别大外显子很重要。我们建议这些序列是大外显子剪接增强子(LESE)。

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