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人类和小鼠中转座元件外显子化的特征。

Characteristics of transposable element exonization within human and mouse.

机构信息

Department of Human Molecular Genetics, Sackler Faculty of Medicine, Tel Aviv University, Tel Aviv, Israel.

出版信息

PLoS One. 2010 Jun 1;5(6):e10907. doi: 10.1371/journal.pone.0010907.

Abstract

Insertion of transposed elements within mammalian genes is thought to be an important contributor to mammalian evolution and speciation. Insertion of transposed elements into introns can lead to their activation as alternatively spliced cassette exons, an event called exonization. Elucidation of the evolutionary constraints that have shaped fixation of transposed elements within human and mouse protein coding genes and subsequent exonization is important for understanding of how the exonization process has affected transcriptome and proteome complexities. Here we show that exonization of transposed elements is biased towards the beginning of the coding sequence in both human and mouse genes. Analysis of single nucleotide polymorphisms (SNPs) revealed that exonization of transposed elements can be population-specific, implying that exonizations may enhance divergence and lead to speciation. SNP density analysis revealed differences between Alu and other transposed elements. Finally, we identified cases of primate-specific Alu elements that depend on RNA editing for their exonization. These results shed light on TE fixation and the exonization process within human and mouse genes.

摘要

转座元件在哺乳动物基因内的插入被认为是哺乳动物进化和物种形成的重要贡献者。转座元件插入内含子可导致它们作为选择性剪接的外显子被激活,这一事件称为外显子化。阐明塑造人类和小鼠蛋白质编码基因中转座元件固定和随后外显子化的进化限制,对于理解外显子化过程如何影响转录组和蛋白质组的复杂性非常重要。在这里,我们表明转座元件的外显子化在人类和小鼠基因中都偏向于编码序列的开始。对单核苷酸多态性 (SNP) 的分析表明,转座元件的外显子化可能具有种群特异性,这意味着外显子化可能增强分化并导致物种形成。SNP 密度分析显示了 Alu 与其他转座元件之间的差异。最后,我们确定了依赖 RNA 编辑进行外显子化的灵长类动物特异性 Alu 元件的情况。这些结果揭示了人类和小鼠基因中转座元件的固定和外显子化过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f053/2879366/a9fffb8cbb7d/pone.0010907.g001.jpg

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