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首页> 外文期刊>Toxicology: An International Journal Concerned with the Effects of Chemicals on Living Systems >An effective antidote for paraquat poisonings: the treatment with lysine acetylsalicylate.
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An effective antidote for paraquat poisonings: the treatment with lysine acetylsalicylate.

机译:百草枯中毒的有效解毒剂:赖氨酸乙酰水杨酸酯治疗。

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摘要

Sodium salicylate (NaSAL) has been shown to have a multifactorial protection mechanism against paraquat (PQ)-induced toxicity, due to its ability to modulate inflammatory signalling systems, to prevent oxidative stress and to its capacity to chelate PQ. Considering that currently there is no pharmaceutical formulation available for parenteral administration of NaSAL, the aim of the present study was to evaluate the antidotal feasibility of a salicylate prodrug, lysine acetylsalicylate (LAS), accessible for parenteral administrations. PQ was administered to Wistar rats by gavage (125mg/kg of PQ ion) and the treatment was performed intraperitoneally with different doses (100, 200 and 400mg/kg of body weight) of LAS. Survival rate was followed during 30 days and living animals at this endpoint were sacrificed for lung, kidney, liver, jejune and heart histological analysis. It was shown, that the salicylate prodrug, LAS, available in a large number of hospitals, is also effective in the treatment of PQ intoxications. From all tested LAS doses, 200mg/kg assured animal's full survival. Comparatively to 60% of mortality observed in PQ only exposed animals, the lethality was higher (80%) in the group that received 400mg/kg of LAS 2h after PQ administration. The dose of 100mg/kg of LAS showed only a modest protection (60% of survival). Collagen deposition was observed by histological analysis in survived animals of all experimental groups, being less pronounced in animals receiving 200mg/kg of LAS, reinforcing the importance of this dose against tissue damage induced by PQ. The results allow us to suggest that LAS should be considered in the hospital treatment of PQ poisonings.
机译:水杨酸钠(NaSAL)由于具有调节炎症信号系统,防止氧化应激和螯合PQ的能力,因此已显示出对百草枯(PQ)诱导的毒性具有多因素保护机制。考虑到目前尚无可用于肠胃外给药的NaSAL药物制剂,本研究的目的是评估可用于肠胃外给药的水杨酸酯前药赖氨酸乙酰水杨酸酯(LAS)的解毒可行性。通过强饲法(125mg / kg PQ离子)向Wistar大鼠施用PQ,并以不同剂量(100、200和400mg / kg体重)LAS腹膜内进行治疗。在30天内追踪存活率,并处死在此终点的活体动物以进行肺,肾,肝,空肠和心脏组织学分析。结果表明,许多医院都可以买到的水杨酸酯前药LAS在治疗PQ中毒方面也很有效。从所有测试的LAS剂量中,200mg / kg可以确保动物的完整存活。与仅暴露于PQ的动物中观察到的死亡率的60%相比,在施用PQ 2h后接受400mg / kg LAS的组中,致死率更高(80%)。 100mg / kg LAS的剂量仅显示了中等程度的保护(生存率的60%)。通过组织学分析在所有实验组的存活动物中观察到胶原蛋白沉积,在接受200mg / kg LAS的动物中不太明显,这增强了该剂量对PQ诱导的组织损伤的重要性。结果使我们建议在医院治疗PQ中毒时应考虑LAS。

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