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From the Cover: Old gene duplication facilitates origin and diversification of an innovative communication system—twice

机译:从封面开始:旧基因复制可促进创新通讯系统的起源和多样化-两次

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摘要

The genetic basis of parallel innovation remains poorly understood due to the rarity of independent origins of the same complex trait among model organisms. We focus on two groups of teleost fishes that independently gained myogenic electric organs underlying electrical communication. Earlier work suggested that a voltage-gated sodium channel gene (Scn4aa), which arose by whole-genome duplication, was neofunctionalized for expression in electric organ and subsequently experienced strong positive selection. However, it was not possible to determine if these changes were temporally linked to the independent origins of myogenic electric organs in both lineages. Here, we test predictions of such a relationship. We show that Scn4aa co-option and rapid sequence evolution were tightly coupled to the two origins of electric organ, providing strong evidence that Scn4aa contributed to parallel innovations underlying the evolutionary diversification of each electric fish group. Independent evolution of electric organs and Scn4aa co-option occurred more than 100 million years following the origin of Scn4aa by duplication. During subsequent diversification of the electrical communication channels, amino acid substitutions in both groups occurred in the same regions of the sodium channel that likely contribute to electric signal variation. Thus, the phenotypic similarities between independent electric fish groups are also associated with striking parallelism at genetic and molecular levels. Our results show that gene duplication can contribute to remarkably similar innovations in repeatable ways even after long waiting periods between gene duplication and the origins of novelty.
机译:平行创新的遗传基础仍然知之甚少,因为模型生物之间具有相同复杂性状的独立起源很少。我们专注于硬骨鱼类的两组,它们独立地获得了构成电通讯的成肌电器官。早期的工作表明,通过全基因组复制产生的电压门控钠通道基因(Scn4aa)被新功能化,可以在电子器官中表达,并随后经历强阳性选择。但是,无法确定这些变化是否在时间上与两个谱系中肌成肌器官的独立起源有关。在这里,我们测试了这种关系的预测。我们表明,Scn4aa的共同选择和快速的序列进化与电子器官的两个起源紧密相关,提供了有力的证据表明Scn4aa促成了每个电子鱼群进化多样化基础的平行创新。在通过复制产生Scn4aa之后,电子器官和Scn4aa共同选择的独立进化发生了超过1亿年。在随后的电通信通道多样化期间,两组中的氨基酸置换均发生在钠通道的相同区域中,这可能会导致电信号变化。因此,独立的电鱼群之间的表型相似性在遗传和分子水平上也与惊人的平行性有关。我们的研究结果表明,即使在基因复制和新颖性来源之间的等待时间过长之后,基因复制也可以以可重复的方式促成非常相似的创新。

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