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Chironex fleckeri (box jellyfish) venom proteins. Expansion of a cnidarian toxin family that elicits variable cytolytic and cardiovascular effects

机译:Chironex fleckeri(盒状水母)毒蛋白。扩展了引起各种溶细胞作用和心血管作用的刺鼻毒素家族

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摘要

The box jellyfish Chironex fleckeri produces extremely potent and rapid-acting venom that is harmful to humans and lethal to prey. Here, we describe the characterization of two C. fleckeri venom proteins, CfTX-A (~40 kDa) and CfTX-B (~42 kDa), which were isolated from C. fleckeri venom using size exclusion chromatography and cation exchange chromatography. Full-length cDNA sequences encoding CfTX-A and -B and a third putative toxin, CfTX-Bt, were subsequently retrieved from a C. fleckeri tentacle cDNA library. Bioinformatic analyses revealed that the new toxins belong to a small family of potent cnidarian pore-forming toxins that includes two other C. fleckeri toxins, CfTX-1 and CfTX-2. Phylogenetic inferences from amino acid sequences of the toxin family grouped CfTX-A, -B, and -Bt in a separate clade from CfTX-1 and -2, suggesting that the C. fleckeri toxins have diversified structurally and functionally during evolution. Comparative bioactivity assays revealed that CfTX-1/2 (25 μg kg^−1) caused profound effects on the cardiovascular system of anesthetized rats, whereas CfTX-A/B elicited only minor effects at the same dose. Conversely, the hemolytic activity of CfTX-A/B (HU50 = 5 ng ml^−1) was at least 30 times greater than that of CfTX-1/2. Structural homology between the cubozoan toxins and insecticidal three-domain Cry toxins (δ-endotoxins) suggests that the toxins have a similar pore-forming mechanism of action involving α-helices of the N-terminal domain, whereas structural diversification among toxin members may modulate target specificity. Expansion of the cnidarian toxin family therefore provides new insights into the evolutionary diversification of box jellyfish toxins from a structural and functional perspective.
机译:盒装水母Chironex fleckeri产生极强力且作用迅速的毒液,对人体有害并致命。在这里,我们描述了使用大小排阻色谱法和阳离子交换色谱法从C. fleckeri毒液分离的两个C. fleckeri毒液蛋白CfTX-A(〜40 kDa)和CfTX-B(〜42 kDa)的表征。随后从弗氏弯曲杆菌触手cDNA文库中检索出编码CfTX-A和-B以及第三种推定毒素CfTX-Bt的全长cDNA序列。生物信息学分析表明,新毒素属于一小类有力的刺胞孔形成毒素,包括另外两种弗雷克氏杆菌毒素CfTX-1和CfTX-2。来自毒素家族氨基酸序列的系统发生推论将CfTX-A,-B和-Bt分组在与CfTX-1和-2分开的分支中,这表明弗雷氏梭菌毒素在进化过程中在结构和功能上均多样化。比较的生物活性分析表明,CfTX-1 / 2(25μgkg ^ -1)对麻醉大鼠的心血管系统产生深远的影响,而CfTX-A / B在相同剂量下仅引起较小的影响。相反,CfTX-A / B(HU50 = 5 ng ml ^ -1)的溶血活性至少是CfTX-1 / 2的30倍。 cubozoan毒素和杀虫三结构域Cry毒素(δ-内毒素)之间的结构同源性表明,该毒素具有类似的形成孔的作用机制,涉及N末端域的α螺旋,而毒素成员之间的结构多样化可能会调节目标特异性。因此,cnidarian毒素家族的扩展从结构和功能的角度为盒状水母毒素的进化多样化提供了新的见解。

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