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The Silent Sway of Splicing by Synonymous Substitutions

机译:同义词替代的无声拼接

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摘要

Alternative splicing diversifies mRNA transcripts in human cells. This sequence-driven process can be influenced greatly by mutations, even those that do not change the protein coding potential of the transcript. Synonymous mutations have been shown to alter gene expression through modulation of splicing, mRNA stability, and translation. Using a synonymous position mutation library in SMN1 exon 7, we show that 23% of synonymous mutations across the exon decrease exon inclusion, suggesting that nucleotide identity across the entire exon has been evolutionarily optimized to support a particular exon inclusion level. Although phylogenetic conservation scores are insufficient to identify synonymous positions important for exon inclusion, an alignment of organisms filtered based on similar exon/intron architecture is highly successful. Although many of the splicing neutral mutations are observed to occur, none of the exon inclusion reducing mutants was found in the filtered alignment. Using the modified phylogenetic comparison as an approach to evaluate the impact on pre-mRNA splicing suggests that up to 45% of synonymous SNPs are likely to alter pre-mRNA splicing. These results demonstrate that coding and pre-mRNA splicing pressures co-evolve and that a modified phylogenetic comparison based on the exon/intron architecture is a useful tool in identifying splice altering SNPs.
机译:选择性剪接使人类细胞中的mRNA转录多样化。该序列驱动的过程可能会受到突变的影响,即使那些不改变转录本蛋白质编码潜能的突变也是如此。已显示同义突变可通过调节剪接,mRNA稳定性和翻译来改变基因表达。在SMN1外显子7中使用同义位置突变库,我们显示了整个外显子中23%的同义突变减少了外显子包涵,这表明整个外显子的核苷酸同一性已得到进化优化,以支持特定的外显子包涵水平。尽管系统发育保守性得分不足以鉴定对于外显子包涵重要的同义位置,但基于相似的外显子/内含子结构过滤的生物的比对非常成功。尽管观察到许多剪接中性突变发生,但在过滤的比对中没有发现外显子包含减少的突变体。使用改良的系统发育比较作为评估对前mRNA剪接的影响的方法表明,高达45%的同义SNP可能会改变前mRNA剪接。这些结果表明编码和前mRNA剪接压力共同发展,并且基于外显子/内含子结构的改良系统发育比较是鉴定剪接改变SNP的有用工具。

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