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蝎螫伤的实验性治疗方案:常见疗法综述及激肽释放酶-激肽抑制剂的作用

Experimental treatment protocols for scorpion envenomation: a review of common therapies and an effect of kallikrein-kinin inhibitors.

作者信息

Ismail M, Fatani A J, Dabees T T

机构信息

Department of Pharmacology, College of Pharmacy, King Saud University, Riyadh, Saudi Arabia.

出版信息

Toxicon. 1992 Oct;30(10):1257-79. doi: 10.1016/0041-0101(92)90442-8.

Abstract

Nine fatal cases from the sting of the scorpion Leiurus quinquestriatus are presented. All victims showed association of CNS and cardiovascular manifestations. Either the CNS or the cardiovascular effects could occur first in the early phases of the scorpion envenoming syndrome; the CNS manifestations, however, always preceded the terminal hypotension and cardiac arrest. Pharmacokinetic studies in rabbits following s.c. injection of the labelled venom showed that rapid absorption took place with about 70% of the maximum blood concentration reached within 15 min. Intramuscular injection of antivenom did not significantly affect the absorption of the venom or the other pharmacokinetic parameters. The total area under concentration time curve was not significantly different from that following i.v. injection, showing that nearly complete absorption of the venom from the s.c. site would occur in 7-8 hr. The i.v. infusion of venom into anaesthetized rats, at a rate comparable to the absorption rate from s.c. sites, allowed the determination of the minimum lethal dose (MLD) with reasonable accuracy. In rescue experiments, anaesthetized rats were injected s.c. with multiple MLD of venom and infused i.v. with drugs commonly used in the treatment of scorpion envenomation. The prepared potent specific antivenoms, but not the commercial polyvalent antivenom, rescued all animals from the lethal effect of the venom, even when injected late. Atropine, atropine+phentolamine, chlorpromazine, hydrocortisone and indomethacin were able, in varying degrees, to rescue some rats injected with 2 MLD of venom. Phentolamine, propranolol, hydralazine and calcium gluconate significantly prolonged the survival time, but did not rescue any animals. Chlorpheniramine, saline and 1/4 saline + 5% dextrose were without any effect. Aprotinin, the kallikrein-kinin inhibitor, was able to rescue half of the animals from the lethal action of the venom. Electrocardiographic studies showed that L. quinquestriatus venom, irrespective of the route of administration, causes myocardial ischaemia and either inferior or anterior wall infarction. This was associated with an initial moderate and a terminal severe bradycardia together with a variety of rhythm and conduction defects. Except for minor and transient electrocardiographic changes, either the prepared antivenoms or aprotinin protected rabbits and rats from the cardiac effects of the venom.

摘要

本文报告了9例由以色列金蝎蜇伤致死的病例。所有受害者均出现中枢神经系统和心血管系统症状。在蝎毒中毒综合征的早期阶段,中枢神经系统或心血管系统的症状可能首先出现;然而,中枢神经系统症状总是先于终末期低血压和心脏骤停出现。对家兔皮下注射标记毒液后的药代动力学研究表明,毒液吸收迅速,在15分钟内达到最大血药浓度的约70%。肌肉注射抗蛇毒血清对毒液的吸收或其他药代动力学参数没有显著影响。浓度-时间曲线下的总面积与静脉注射后的情况无显著差异,表明皮下注射部位的毒液在7-8小时内几乎完全吸收。以与皮下注射部位吸收速率相当的速度向麻醉大鼠静脉输注毒液,可以较为准确地测定最小致死剂量(MLD)。在救援实验中,给麻醉大鼠皮下注射多个MLD的毒液,并静脉输注常用于治疗蝎毒中毒的药物。制备的高效特异性抗蛇毒血清,而非市售的多价抗蛇毒血清,即使注射较晚,也能使所有动物从毒液的致死作用中获救。阿托品、阿托品+酚妥拉明、氯丙嗪、氢化可的松和吲哚美辛在不同程度上能够挽救一些注射了2 MLD毒液的大鼠。酚妥拉明、普萘洛尔、肼屈嗪和葡萄糖酸钙显著延长了存活时间,但未能挽救任何动物。氯苯那敏(扑尔敏)、生理盐水和1/4生理盐水+5%葡萄糖没有任何作用。激肽释放酶-激肽抑制剂抑肽酶能够使一半的动物从毒液的致死作用中获救。心电图研究表明,无论给药途径如何,以色列金蝎毒液都会导致心肌缺血以及下壁或前壁梗死。这与最初的中度和终末期严重心动过缓以及各种节律和传导异常有关。除了轻微和短暂的心电图变化外,制备的抗蛇毒血清或抑肽酶均可保护家兔和大鼠免受毒液对心脏的影响。

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