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古老毒液的演变:刺胞动物毒素新家族的识别以及海葵钠离子和钾离子神经毒素的共同进化起源。

Evolution of an ancient venom: recognition of a novel family of cnidarian toxins and the common evolutionary origin of sodium and potassium neurotoxins in sea anemone.

机构信息

Venom Evolution Laboratory, School of Biological Sciences, The University of Queensland, St. Lucia, Queensland, Australia Institute for Molecular Bioscience, The University of Queensland, St. Lucia, Queensland, Australia.

Department of Ecology, Evolution and Behavior, The Alexander Silberman Institute for Life Sciences, Hebrew University of Jerusalem, Jerusalem, Israel.

出版信息

Mol Biol Evol. 2015 Jun;32(6):1598-610. doi: 10.1093/molbev/msv050. Epub 2015 Mar 9.

Abstract

Despite Cnidaria (sea anemones, corals, jellyfish, and hydroids) being the oldest venomous animal lineage, structure-function relationships, phyletic distributions, and the molecular evolutionary regimes of toxins encoded by these intriguing animals are poorly understood. Hence, we have comprehensively elucidated the phylogenetic and molecular evolutionary histories of pharmacologically characterized cnidarian toxin families, including peptide neurotoxins (voltage-gated Na(+) and K(+) channel-targeting toxins: NaTxs and KTxs, respectively), pore-forming toxins (actinoporins, aerolysin-related toxins, and jellyfish toxins), and the newly discovered small cysteine-rich peptides (SCRiPs). We show that despite long evolutionary histories, most cnidarian toxins remain conserved under the strong influence of negative selection-a finding that is in striking contrast to the rapid evolution of toxin families in evolutionarily younger lineages, such as cone snails and advanced snakes. In contrast to the previous suggestions that implicated SCRiPs in the biomineralization process in corals, we demonstrate that they are potent neurotoxins that are likely involved in the envenoming function, and thus represent the first family of neurotoxins from corals. We also demonstrate the common evolutionary origin of type III KTxs and NaTxs in sea anemones. We show that type III KTxs have evolved from NaTxs under the regime of positive selection, and likely represent a unique evolutionary innovation of the Actinioidea lineage. We report a correlation between the accumulation of episodically adaptive sites and the emergence of novel pharmacological activities in this rapidly evolving neurotoxic clade.

摘要

尽管刺胞动物(海葵、珊瑚、水母和水螅)是最古老的有毒动物谱系,但这些迷人动物的毒素结构-功能关系、系统发生分布和分子进化机制仍知之甚少。因此,我们全面阐明了具有药理学特征的刺胞动物毒素家族的系统发生和分子进化历史,包括肽神经毒素(电压门控 Na(+)和 K(+)通道靶向毒素:NaTx 和 KTx)、孔形成毒素(肌动蛋白孔毒素、aerolysin 相关毒素和水母毒素)以及新发现的小半胱氨酸丰富肽(SCRiPs)。我们表明,尽管具有悠久的进化历史,但大多数刺胞动物毒素在强烈的负选择影响下仍然保持保守——这一发现与进化较年轻谱系(如锥形蜗牛和高级蛇类)中毒素家族的快速进化形成鲜明对比。与先前暗示 SCRiPs 参与珊瑚生物矿化过程的观点相反,我们证明它们是有效的神经毒素,可能参与了毒液功能,因此代表了珊瑚中的第一类神经毒素。我们还证明了海葵中 III 型 KTx 和 NaTx 的共同进化起源。我们表明,III 型 KTx 是在正选择的作用下从 NaTx 进化而来的,可能代表了 Actinioidea 谱系的独特进化创新。我们报告了在这个快速进化的神经毒性类群中,偶发性适应性位点的积累与新的药理学活性的出现之间存在相关性。

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