首页> 外文期刊>Protein Science: A Publication of the Protein Society >Elucidation of the solution structure of cardiotoxin analogue V from the Taiwan cobra (Naja naja atra)--identification of structural features important for the lethal action of snake venom cardiotoxins.
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Elucidation of the solution structure of cardiotoxin analogue V from the Taiwan cobra (Naja naja atra)--identification of structural features important for the lethal action of snake venom cardiotoxins.

机译:阐明台湾眼镜蛇(Naja naja atra)的心脏毒素类似物V的溶液结构-鉴定对蛇毒心脏毒素有致死作用的重要结构特征。

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The aim of the present study is to understand the structural features responsible for the lethal activity of snake venom cardiotoxins. Comparison of the lethal potency of the five cardiotoxin isoforms isolated from the venom of Taiwan cobra (Naja naja atra) reveals that the lethal potency of CTX I and CTX V are about twice of that exhibited by CTX II, CTX III, and CTX IV. In the present study, the solution structure of CTX V has been determined at high resolution using multidimensional proton NMR spectroscopy and dynamical simulated annealing techniques. Comparison of the high resolution solution structures of CTX V with that of CTX IV reveals that the secondary structural elements in both the toxin isoforms consist of a triple and double-stranded antiparallel beta-sheet domains. Critical examination of the three-dimensional structure of CTX V shows that the residues at the tip of Loop III form a distinct "finger-shaped" projection comprising of nonpolar residues. The occurrence of the nonpolar "finger-shaped" projection leads to the formation of a prominent cleft between the residues located at the tip of Loops II and III. Interestingly, the occurrence of a backbone hydrogen bonding (Val27CO to Leu48NH) in CTX IV is found to distort the "finger-shaped" projection and consequently diminish the cleft formation at the tip of Loops II and III. Comparison of the solution structures and lethal potencies of other cardiotoxin isoforms isolated from the Taiwan cobra (Naja naja atra) venom shows that a strong correlation exists between the lethal potency and occurrence of the nonpolar "finger-shaped" projection at the tip of Loop III. Critical analysis of the structures of the various CTX isoforms from the Taiwan cobra suggest that the degree of exposure of the cationic charge (to the solvent) contributed by the invariant lysine residue at position 44 on the convex side of the CTX molecules could be another crucial factor governing their lethal potency.
机译:本研究的目的是了解负责蛇毒心毒素的致死活性的结构特征。比较从台湾眼镜蛇毒(Naja naja atra)毒液中分离出来的五种心脏毒素同工型的致死力,发现CTX I和CTX V的致死力约为CTX II,CTX III和CTX IV的两倍。在本研究中,已使用多维质子NMR光谱和动态模拟退火技术以高分辨率确定了CTX V的溶液结构。 CTX V和CTX IV的高分辨率溶液结构的比较表明,两种毒素同工型中的二级结构元素均由三链和双链反平行β-折叠结构域组成。对CTX V三维结构的严格检查表明,Loop III末端的残基形成了一个由非极性残基组成的独特的“手指状”突起。非极性“手指形”投影的出现导致在Loops II和III尖端处的残基之间形成明显的裂缝。有趣的是,发现在CTX IV中出现主链氢键(Val27CO与Leu48NH)扭曲了“手指形”的突出部分,从而减少了Loop II和III尖端的裂缝形成。从台湾眼镜蛇(Naja naja atra)毒液分离的其他心脏毒素同工型的溶液结构和致死力的比较表明,致死力与环III末端非极性“手指形”投射的发生之间存在很强的相关性。对来自台湾眼镜蛇的各种CTX同工型的结构的关键分析表明,CTX分子凸侧第44位不变的赖氨酸残基对阳离子电荷(暴露于溶剂)的影响程度可能是另一个关键因素。决定他们致命能力的因素。

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