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Bioscavenger 可作为经皮染毒VX 中毒后的延迟治疗干预措施在豚鼠中有效。

Bioscavenger is effective as a delayed therapeutic intervention following percutaneous VX poisoning in the guinea-pig.

机构信息

CBR, Dstl Porton Down, UK.

CBR, Dstl Porton Down, UK.

出版信息

Toxicol Lett. 2018 Sep 1;293:198-206. doi: 10.1016/j.toxlet.2017.11.029. Epub 2017 Nov 26.

Abstract

The prolonged systemic exposure that follows skin contamination with low volatility nerve agents, such as VX, requires treatment to be given over a long time due to the relatively short half-lives of the therapeutic compounds used. Bioscavengers, such as butyrylcholinesterase (BChE), have been shown to provide effective post-exposure protection against percutaneous nerve agent when given immediately on signs of poisoning and to reduce reliance on additional treatments. In order to assess the benefits of administration of bioscavenger at later times, its effectiveness was assessed when administration was delayed for 2h after the appearance of signs of poisoning in guinea-pigs challenged with VX (4×LD). VX-challenged animals received atropine, HI-6 and avizafone on signs of poisoning and 2h later the same combination with or without bioscavenger. Five out of 6 animals which received BChE 2h after the appearance of signs of poisoning survived to the end of the study at 48h, compared with 6 out of 6 which received BChE immediately on signs. All the animals (n=6+6) that received only MedCM, without the addition of BChE, died within 10h of poisoning. The toxicokinetics of a sub-lethal challenge of percutaneous VX were determined in untreated animals. Blood VX concentration peaked at approximately 4h after percutaneous dosing with 0.4×LD; VX was still detectable at 36h and had declined to levels below the lower limit of quantification (10pg/mL) by 48h in 7 of 8 animals, with the remaining animal having a concentration of 12pg/mL. These studies confirm the persistent systemic exposure to nerve agent following percutaneous poisoning and demonstrate that bioscavenger can be an effective component of treatment even if its administration is delayed.

摘要

皮肤接触低挥发性神经毒剂(如 VX)后会导致长时间的全身性暴露,由于所用治疗化合物的半衰期相对较短,因此需要长时间进行治疗。生物清除剂(如丁酰胆碱酯酶(BChE))已被证明在中毒迹象出现时立即给予,可以提供针对经皮神经毒剂的有效暴露后保护,并减少对其他治疗方法的依赖。为了评估在较晚时间给予生物清除剂的益处,在挑战 VX(4×LD)的豚鼠出现中毒迹象后 2 小时延迟给药时,评估了其有效性。接受 VX 挑战的动物在出现中毒迹象时接受了阿托品、HI-6 和阿维佐凡,2 小时后,在相同的组合中加入或不加入生物清除剂。在出现中毒迹象后 2 小时接受 BChE 治疗的 5 只动物中有 5 只存活到研究结束(48 小时),而在出现中毒迹象时立即接受 BChE 治疗的 6 只动物中有 6 只存活。仅接受 MedCM 治疗(未添加 BChE)的所有动物(n=6+6)在中毒后 10 小时内死亡。在未治疗的动物中,确定了经皮 VX 亚致死挑战的毒代动力学。经皮给药 0.4×LD 后,血液 VX 浓度约在 4 小时时达到峰值;在 36 小时时仍可检测到 VX,在 48 小时时,8 只动物中有 7 只的浓度下降到低于定量下限(10pg/mL),而其余 1 只动物的浓度为 12pg/mL。这些研究证实了经皮中毒后持续的全身性神经毒剂暴露,并表明生物清除剂即使在延迟给药的情况下也可以成为治疗的有效组成部分。

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