Venom-Induced Blood Disturbances by Palearctic Viperid Snakes, and Their Relative Neutralization by Antivenoms and Enzyme-Inhibitors

被引:25
作者
Chowdhury, Abhinandan [1 ,2 ]
Zdenek, Christina N. [1 ]
Lewin, Matthew R. [3 ,4 ]
Carter, Rebecca [4 ]
Jagar, Tomaz
Ostanek, Erika
Harjen, Hannah [5 ]
Aldridge, Matt [6 ]
Soria, Raul [7 ]
Haw, Grace [1 ]
Fry, Bryan G. [1 ]
机构
[1] Univ Queensland, Sch Biol Sci, Venom Evolut Lab, St Lucia, Qld, Australia
[2] North South Univ, Dept Biochem & Microbiol, Dhaka, Bangladesh
[3] Calif Acad Sci, San Francisco, CA 94118 USA
[4] Ophirex Inc, Corte Madera, CA USA
[5] Norwegian Univ Life Sci, Dept Compan Anim Clin Sci, As, Norway
[6] MicroPharm Ltd, Newcastle Emlyn, Wales
[7] Inosan Biopharma, Madrid, Spain
基金
澳大利亚研究理事会;
关键词
venom; antivenom; enzyme inhibition; coagulopathy; snakebite; AMMODYTES-AMMODYTES; BERUS-BERUS; PROCOAGULANT TOXICITY; CLINICAL-IMPLICATIONS; METALLOPROTEINASE; DIVERSIFICATION; MONTIVIPERA; SNAKEBITES; EFFICACY; BITES;
D O I
10.3389/fimmu.2021.688802
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Palearctic vipers are medically significant snakes in the genera Daboia, Macrovipera, Montivipera, and Vipera which occur throughout Europe, Central Asia, Near and Middle East. While the ancestral condition is that of a small-bodied, lowland species, extensive diversification has occurred in body size, and niche specialization. Using 27 venom samples and a panel of in vitro coagulation assays, we evaluated the relative coagulotoxic potency of Palearctic viper venoms and compared their neutralization by three antivenoms (Insoserp Europe, VIPERFAV and ViperaTAb) and two metalloprotease inhibitors (prinomastat and DMPS). We show that variation in morphology parallels variation in the Factor X activating procoagulant toxicity, with the three convergent evolutions of larger body sizes (Daboia genus, Macrovipera genus, and Vipera ammodytes uniquely within the Vipera genus) were each accompanied by a significant increase in procoagulant potency. In contrast, the two convergent evolutions of high altitude specialization (the Montivipera genus and Vipera latastei uniquely within the Vipera genus) were each accompanied by a shift away from procoagulant action, with the Montivipera species being particularly potently anticoagulant. Inoserp Europe and VIPERFAV antivenoms were both effective against a broad range of Vipera species, with Inoserp able to neutralize additional species relative to VIPERFAV, reflective of its more complex antivenom immunization mixture. In contrast, ViperaTAb was extremely potent in neutralizing V. berus but, reflective of this being a monovalent antivenom, it was not effective against other Vipera species. The enzyme inhibitor prinomastat efficiently neutralized the metalloprotease-driven Factor X activation of the procoagulant venoms. In contrast, DMPS (2,3-dimercapto-1-propanesulfonic acid), which as been suggested as another potential treatment option in the absence of antivenom, DMPS failed against all venoms tested. Overall, our results highlight the evolutionary variations within Palearctic vipers and help to inform clinical management of viper envenomation.
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页数:14
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