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The intrinsic dimension of protein sequence evolution

机译:蛋白质序列进化的内在维度

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摘要

It is well known that, in order to preserve its structure and function, a protein cannot change its sequence at random, but only by mutations occurring preferentially at specific locations. We here investigate quantitatively the amount of variability that is allowed in protein sequence evolution, by computing the intrinsic dimension (ID) of the sequences belonging to a selection of protein families. The ID is a measure of the number of independent directions that evolution can take starting from a given sequence. We find that the ID is practically constant for sequences belonging to the same family, and moreover it is very similar in different families, with values ranging between 6 and 12. These values are significantly smaller than the raw number of amino acids, confirming the importance of correlations between mutations in different sites. However, we demonstrate that correlations are not sufficient to explain the small value of the ID we observe in protein families. Indeed, we show that the ID of a set of protein sequences generated by maximum entropy models, an approach in which correlations are accounted for, is typically significantly larger than the value observed in natural protein families. We further prove that a critical factor to reproduce the natural ID is to take into consideration the phylogeny of sequences.
机译:众所周知,为了保持其结构和功能,蛋白质不能随机改变其序列,而只能通过优先发生在特定位置的突变来改变。我们在这里通过计算属于蛋白质家族选择的序列的内在尺寸(ID),定量研究蛋白质序列进化中允许的变异量。 ID是度量从给定序列开始可以采取的独立方向数量的度量。我们发现,对于同一家族的序列,ID实际上是恒定的,而且在不同家族中,ID非常相似,其值在6到12之间。这些值显着小于氨基酸的原始数目,从而确认了重要性不同位点突变之间的相关性。但是,我们证明了相关性不足以解释我们在蛋白质家族中观察到的ID的较小值。实际上,我们证明了由最大熵模型(一种考虑了相关性的方法)生成的一组蛋白质序列的ID通常明显大于在天然蛋白质家族中观察到的值。我们进一步证明,重现天然ID的关键因素是要考虑序列的系统发育。

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