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可变剪接与基因复制的(非)依赖性

The (in)dependence of alternative splicing and gene duplication.

作者信息

Talavera David, Vogel Christine, Orozco Modesto, Teichmann Sarah A, de la Cruz Xavier

机构信息

Molecular Modeling and Bioinformatics Unit, Parc Científic de Barcelona, Barcelona, Spain.

出版信息

PLoS Comput Biol. 2007 Mar 2;3(3):e33. doi: 10.1371/journal.pcbi.0030033.

Abstract

Alternative splicing (AS) and gene duplication (GD) both are processes that diversify the protein repertoire. Recent examples have shown that sequence changes introduced by AS may be comparable to those introduced by GD. In addition, the two processes are inversely correlated at the genomic scale: large gene families are depleted in splice variants and vice versa. All together, these data strongly suggest that both phenomena result in interchangeability between their effects. Here, we tested the extent to which this applies with respect to various protein characteristics. The amounts of AS and GD per gene are anticorrelated even when accounting for different gene functions or degrees of sequence divergence. In contrast, the two processes appear to be independent in their influence on variation in mRNA expression. Further, we conducted a detailed comparison of the effect of sequence changes in both alternative splice variants and gene duplicates on protein structure, in particular the size, location, and types of sequence substitutions and insertions/deletions. We find that, in general, alternative splicing affects protein sequence and structure in a more drastic way than gene duplication and subsequent divergence. Our results reveal an interesting paradox between the anticorrelation of AS and GD at the genomic level, and their impact at the protein level, which shows little or no equivalence in terms of effects on protein sequence, structure, and function. We discuss possible explanations that relate to the order of appearance of AS and GD in a gene family, and to the selection pressure imposed by the environment.

摘要

可变剪接(AS)和基因复制(GD)都是使蛋白质组多样化的过程。最近的例子表明,AS引入的序列变化可能与GD引入的序列变化相当。此外,这两个过程在基因组水平上呈负相关:大基因家族中的剪接变体较少,反之亦然。总之,这些数据有力地表明,这两种现象在其作用上具有互换性。在这里,我们测试了这在各种蛋白质特征方面的适用程度。即使考虑到不同的基因功能或序列差异程度,每个基因的AS和GD量也是负相关的。相比之下,这两个过程对mRNA表达变化的影响似乎是独立的。此外,我们对可变剪接变体和基因复制产物中的序列变化对蛋白质结构的影响进行了详细比较,特别是序列替换和插入/缺失的大小、位置和类型。我们发现,一般来说,可变剪接对蛋白质序列和结构的影响比基因复制及随后的分化更为剧烈。我们的结果揭示了基因组水平上AS和GD的负相关与其在蛋白质水平上的影响之间存在一个有趣的矛盾,即它们对蛋白质序列、结构和功能的影响几乎没有等效性。我们讨论了与基因家族中AS和GD出现顺序以及环境施加的选择压力相关的可能解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2096/1847985/52fdf6251bc1/pcbi.0030033.g001.jpg

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