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新型同源二聚体三指神经毒素的结构与功能表征,该毒素来源于 Ophiophagus hannah(眼镜王蛇)的毒液。

Structural and functional characterization of a novel homodimeric three-finger neurotoxin from the venom of Ophiophagus hannah (king cobra).

机构信息

Department of Biological Sciences, National University of Singapore, Singapore.

出版信息

J Biol Chem. 2010 Mar 12;285(11):8302-15. doi: 10.1074/jbc.M109.074161. Epub 2010 Jan 13.

Abstract

Snake venoms are a mixture of pharmacologically active proteins and polypeptides that have led to the development of molecular probes and therapeutic agents. Here, we describe the structural and functional characterization of a novel neurotoxin, haditoxin, from the venom of Ophiophagus hannah (King cobra). Haditoxin exhibited novel pharmacology with antagonism toward muscle (alphabetagammadelta) and neuronal (alpha(7), alpha(3)beta(2), and alpha(4)beta(2)) nicotinic acetylcholine receptors (nAChRs) with highest affinity for alpha(7)-nAChRs. The high resolution (1.5 A) crystal structure revealed haditoxin to be a homodimer, like kappa-neurotoxins, which target neuronal alpha(3)beta(2)- and alpha(4)beta(2)-nAChRs. Interestingly however, the monomeric subunits of haditoxin were composed of a three-finger protein fold typical of curaremimetic short-chain alpha-neurotoxins. Biochemical studies confirmed that it existed as a non-covalent dimer species in solution. Its structural similarity to short-chain alpha-neurotoxins and kappa-neurotoxins notwithstanding, haditoxin exhibited unique blockade of alpha(7)-nAChRs (IC(50) 180 nm), which is recognized by neither short-chain alpha-neurotoxins nor kappa-neurotoxins. This is the first report of a dimeric short-chain alpha-neurotoxin interacting with neuronal alpha(7)-nAChRs as well as the first homodimeric three-finger toxin to interact with muscle nAChRs.

摘要

蛇毒是一种药理学上活跃的蛋白质和多肽混合物,这些物质促进了分子探针和治疗剂的发展。在这里,我们描述了来自 Ophiophagus hannah(眼镜王蛇)毒液的一种新型神经毒素 haditoxin 的结构和功能特征。Haditoxin 表现出新型药理学特性,对肌肉(alphabetagammadelta)和神经元(alpha(7)、alpha(3)beta(2)和 alpha(4)beta(2))烟碱型乙酰胆碱受体(nAChRs)具有拮抗作用,对 alpha(7)-nAChRs 的亲和力最高。高分辨率(1.5 A)晶体结构显示,Haditoxin 像 kappa-神经毒素一样是同源二聚体,可靶向神经元 alpha(3)beta(2)-和 alpha(4)beta(2)-nAChRs。然而,有趣的是,Haditoxin 的单体亚基由三指蛋白折叠组成,这是一种典型的拟除虫菊酯短链 alpha-神经毒素。生化研究证实,它在溶液中以非共价二聚体形式存在。尽管其结构与短链 alpha-神经毒素和 kappa-神经毒素相似,但 Haditoxin 对 alpha(7)-nAChRs 的独特阻断作用(IC(50) 180nm)既不受短链 alpha-神经毒素也不受 kappa-神经毒素的识别。这是第一个报道的与神经元 alpha(7)-nAChRs 相互作用的二聚体短链 alpha-神经毒素,也是第一个与肌肉 nAChRs 相互作用的同源二聚体三指毒素。

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