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首页> 外文期刊>Human and Experimental Toxicology >Clinical manifestations of VX poisoning following percutaneous exposure in the domestic white pig.
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Clinical manifestations of VX poisoning following percutaneous exposure in the domestic white pig.

机译:家养白猪经皮暴露后VX中毒的临床表现。

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摘要

Nerve agents are a class of organophosphorus chemicals that inhibit certain cholinesterase enzymes (ChE). If untreated, percutaneous exposure to nerve agents, such as VX (O-ethyl-S-[2(diisopropylamino)ethyl] methylphosphonothioate) can cause paralysis, apnoea and death. Much of the information concerning the percutaneous absorption and subsequent toxicity of nerve agents has been obtained using various rodent models. However, the most relevant 'skin model' is arguably the pig. Therefore, the purpose of this study was to examine the clinical manifestations of VX intoxication in the domestic white pig following a 2 LD50 (120 microg/kg) percutaneous challenge. There was a consistent onset of signs (where present) in each animal: mastication was followed by miosis, salivation, fasciculations and apnoea. Whilst ChE activity did not correlate with the onset of signs, there was a qualitative relationship in that mastication preceded substantial ChE inhibition, miosis lagged behind the linear decrease in acetylcholinesterase (AChE) activity and fasciculations and apnoea occurred after maximum ChE inhibition had been attained (5-10% of normal). These observations may be of use for the triage of patients exposed to VX. In comparison with similar studies with GD, VX did not affect glucose utilization. However, VX was similar to GD in that it caused a mild hyperkalaemia and hyperphosphataemia, although the significance of this observation was not clear. There was substantial lateral diffusion of the initial droplet of VX over the application site, indicating that, when decontaminating exposed skin, attention should also be directed to areas peripheral to the original site of exposure.
机译:神经药物是一类可抑制某些胆碱酯酶(ChE)的有机磷化学物质。如果不进行治疗,经皮接触神经毒剂,例如VX(O-乙基-S- [2(二异丙基氨基)乙基]甲基硫代磷酸膦酸酯)会引起麻痹,呼吸暂停和死亡。使用各种啮齿动物模型已经获得了许多有关神经制剂经皮吸收和随后毒性的信息。但是,最相关的“皮肤模型”可以说是猪。因此,本研究的目的是检查经皮2 LD50(120 microg / kg)攻击后家养白猪中VX中毒的临床表现。每只动物均出现一致的体征(如果有的话):咀嚼后出现瞳孔缩小,流涎,束缚和呼吸暂停。尽管ChE的活性与体征的发作无关,但存在一定的定性关系,即咀嚼先于大量的ChE抑制,而瞳孔缩小则落后于乙酰胆碱酯酶(AChE)活性的线性下降,并且在达到最大ChE抑制作用后发生了束缚和呼吸暂停(正常的5-10%)。这些观察结果可用于对暴露于VX的患者进行分类。与GD的类似研究相比,VX不会影响葡萄糖利用率。但是,VX与GD相似,因为它引起了轻度的高钾血症和高磷血症,尽管这一观察的意义尚不清楚。 VX的初始液滴在涂抹部位上有大量的横向扩散,这表明在对裸露的皮肤进行消毒时,还应注意原始暴露部位周围的区域。

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