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Resolving the ortholog conjecture: orthologs tend to be weakly, but significantly, more similar in function than paralogs.

机译:解决直系同源物猜想:直系同源物往往较弱,但与旁系同源物功能相似。

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摘要

The function of most proteins is not determined experimentally, but is extrapolated from homologs. According to the "ortholog conjecture", or standard model of phylogenomics, protein function changes rapidly after duplication, leading to paralogs with different functions, while orthologs retain the ancestral function. We report here that a comparison of experimentally supported functional annotations among homologs from 13 genomes mostly supports this model. We show that to analyze GO annotation effectively, several confounding factors need to be controlled: authorship bias, variation of GO term frequency among species, variation of background similarity among species pairs, and propagated annotation bias. After controlling for these biases, we observe that orthologs have generally more similar functional annotations than paralogs. This is especially strong for sub-cellular localization. We observe only a weak decrease in functional similarity with increasing sequence divergence. These findings hold over a large diversity of species; notably orthologs from model organisms such as E. coli, yeast or mouse have conserved function with human proteins.
机译:大多数蛋白质的功能不是通过实验确定的,而是从同源物推断出来的。根据“直系同源物推测”或系统发育组学的标准模型,蛋白质功能在复制后迅速改变,导致旁系同源物具有不同的功能,而直系同源物保留祖先功能。我们在这里报告,从13个基因组的同源物中实验支持的功能注释的比较主要支持此模型。我们表明,要有效地分析GO注释,需要控制几个混淆因素:作者偏见,GO物种之间的术语频率变化,物种对之间的背景相似性变化以及传播的注释偏差。在控制了这些偏差之后,我们观察到直系同源物通常比旁系同源物具有更多相似的功能注释。这对于亚细胞定位特别强。我们观察到功能相似性随序列差异的增加而仅微弱下降。这些发现涵盖了种类繁多的物种。值得注意的是,来自模型生物(例如大肠杆菌,酵母或小鼠)的直系同源物与人蛋白具有保守的功能。

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