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Adaptive evolution of distinct prey-specific toxin genes in rear-fanged snake venom

机译:左右蛇毒液中不同捕食特异性毒素基因的自适应演变

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摘要

Venom proteins evolve rapidly, and as a trophic adaptation are excellent models for predator-prey evolutionary studies. The key to a deeper understanding of venom evolution is an integrated approach, combining prey assays with analysis of venom gene expression and venom phenotype. Here, we use such an approach to study venom evolution in the Amazon puffing snake, Spilotes sulphureus, a generalist feeder. We identify two novel three-finger toxins: sulditoxin and sulmotoxin 1. These new toxins are not only two of the most abundant venomproteins, but are also functionally intriguing, displaying distinct prey-specific toxicities. Sulditoxin is highly toxic towards lizard prey, but is non-toxic towards mammalian prey, even at greater than 22-fold higher dosage. By contrast, sulmotoxin 1 exhibits the reverse trend. Furthermore, evolutionary analysis and structural modelling show highest sequence variability in the central loop of these proteins, probably driving taxon-specific toxicity. This is, to our knowledge, the first case in which a bimodal and contrasting pattern of toxicity has been shown for proteins in the venom of a single snake in relation to diet. Our study is an example of how toxin gene neofunctionalization can result in a venom system dominated by one protein superfamily and still exhibit flexibility in prey capture efficacy.
机译:毒液蛋白迅速发展,作为营养性适应是捕食者 - 猎物进化研究的优秀模型。更深入地理解毒液进化的关键是一种综合方法,与毒液基因表达和毒液表型分析相结合的猎物测定。在这里,我们使用这种方法来研究亚马逊膨化蛇的毒液进化,Spilotes Sulphureus,一般饲养者。我们鉴定了两种新型三指毒素:苏硝辛和磺毒素1.这些新的毒素不仅是最丰富的毒液蛋白的两个,而且也是在功能上有趣的,显示不同的特异性胃肠毒性。苏硝辛对蜥蜴猎物具有浓重的毒性,但对于哺乳动物猎物无毒,甚至在更高的剂量上较高。相比之下,磺毒素1表现出反向趋势。此外,进化分析和结构建模在这些蛋白质的中央循环中显示出最高的序列变异性,可能导致分类群特异性毒性。对我们的知识,这是第一种情况,其中已经显示了与饮食有关的单个蛇的毒液中蛋白质的双峰和对比模式的毒性。我们的研究是如何产生毒素的毒素系统可以导致由一种蛋白质超家族主导的毒液系统,并且仍然表现出捕食性捕获功效的灵活性。

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