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蛇毒磷脂酶A2(Vipoxin)及其组分的急性毒性:酸性组分是PLA2毒性的“抑制剂”吗?

Acute toxicity of vipoxin and its components: is the acidic component an "inhibitor" of PLA2 toxicity?

作者信息

Atanasov Vasil N, Stoykova Silviya, Goranova Yana, Mitewa Mariana, Petrova Svetla

机构信息

Sofia University "St. Kl. Ohridski", Faculty of Chemistry and Pharmacy, Department of Analytical Chemistry, Laboratory of Biocoordination and Bioanalytical Chemitsry, Sofia, Bulgaria ; Military Medical Academy, Emergency Toxicology Clinic, Sofia, Bulgaria.

出版信息

Interdiscip Toxicol. 2012 Dec;5(4):169-72. doi: 10.2478/v10102-012-0028-z.

Abstract

Vipoxin is a heterodimeric neurotoxin isolated from the venom of the Bulgarian long-nosed viper Vipera ammodytes meridionalis. Vipoxin represents a noncovalent association of two subunits - a basic and toxic phospholipase A2 enzyme, and an acidic non-enzymatic component (vipoxin's acidic component). It was postulated that the phospholipase A2 subunit was more toxic than the whole vipoxin complex and the function of the acidic component was to reduce the enzymatic and toxic activities of the basic phospholipase A2. In the present study, we report new data on the acute toxicity (LD50) of vipoxin and its individual separated components. Vipoxin LD50 (mice, i.p. and i.v.) values were found to be 0.7-1.2 mg/kg b.w. (i.p.) and 0.9-1.3 mg/kg b.w. (i.v.). The established LD50 values for the separated pure phospholipase A2 subunit are higher - 10.0-13.0 mg/kg b.w (i.p.) and 2.2-3.0 mg/kg b.w. (i.v.), i.e. the individual phospholipase A2 subunit displays less toxic activity than vipoxin, contrary to the data published in the literature. The reconstituted vipoxin complex (obtained after preliminary incubation of pure separated phospholipase A2 and acidic component showed enzyme activity and toxicity comparable to that of the native vipoxin complex. Addition of acidic component to the phospholipase A2 subunit showed a positive effect on the enzymatic activity, reaching maximal enzyme reaction rate of acidic component to phospholipase A2 molar ratio of 0.8:1 on using 4-nitro-3-octanoyloxy-benzoic acid as substrate. For the first time we showed that the acidic subunit was absolutely required for the toxic activity of vipoxin. Based on the obtained results, we assume that the function of the acidic component is to stabilize the neurotoxin's quaternary structure, required for its toxic and enzymatic activities, similarly to the role of the acidic component of crotoxin.

摘要

蝰蛇毒素是从保加利亚长鼻蝰蛇(Vipera ammodytes meridionalis)毒液中分离出的一种异源二聚体神经毒素。蝰蛇毒素是由两个亚基通过非共价结合而成——一个碱性且有毒的磷脂酶A2酶,以及一个酸性非酶成分(蝰蛇毒素的酸性成分)。据推测,磷脂酶A2亚基比整个蝰蛇毒素复合物毒性更强,而酸性成分的作用是降低碱性磷脂酶A2的酶活性和毒性。在本研究中,我们报告了蝰蛇毒素及其单独分离成分的急性毒性(半数致死量,LD50)的新数据。蝰蛇毒素的LD50(小鼠,腹腔注射和静脉注射)值分别为0.7 - 1.2毫克/千克体重(腹腔注射)和0.9 - 1.3毫克/千克体重(静脉注射)。分离得到的纯磷脂酶A2亚基的既定LD50值更高——10.0 - 13.0毫克/千克体重(腹腔注射)和2.2 - 3.0毫克/千克体重(静脉注射),即单独的磷脂酶A2亚基显示出比蝰蛇毒素更低的毒性活性,这与文献中发表的数据相反。重组的蝰蛇毒素复合物(在将纯分离的磷脂酶A2和酸性成分进行预孵育后获得)显示出与天然蝰蛇毒素复合物相当的酶活性和毒性。向磷脂酶A2亚基添加酸性成分对酶活性有积极影响,以4 - 硝基 - 3 - 辛酰氧基 - 苯甲酸为底物时,酸性成分与磷脂酶A2的摩尔比为0.8:1时达到最大酶反应速率。我们首次表明酸性亚基是蝰蛇毒素毒性活性绝对必需的。基于所获得的结果,我们推测酸性成分的功能是稳定神经毒素的四级结构,这是其毒性和酶活性所必需的,类似于响尾蛇毒素酸性成分的作用。

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本文引用的文献

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Structure of the neurotoxic complex vipoxin at 1.4 A resolution.神经毒性复合物蛇毒神经毒素在1.4埃分辨率下的结构。
Acta Crystallogr D Biol Crystallogr. 2001 Nov;57(Pt 11):1552-9. doi: 10.1107/s0907444901013543. Epub 2001 Oct 25.
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An aqueous endpoint assay of snake venom phospholipase A2.蛇毒磷脂酶A2的水性终点测定法。
Toxicon. 1996 Oct;34(10):1149-55. doi: 10.1016/0041-0101(96)00057-8.
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Comparison of crotoxin isoforms reveals that stability of the complex plays a major role in its pharmacological action.
Eur J Biochem. 1993 Jun 1;214(2):491-6. doi: 10.1111/j.1432-1033.1993.tb17946.x.
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Model for the interaction of crotoxin, a phospholipase A2 neurotoxin, with presynaptic membranes.
Biochemistry. 1993 Oct 12;32(40):10708-13. doi: 10.1021/bi00091a022.

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