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首页> 外文期刊>Toxicology Letters: An International Journal Providing a Forum for Original and Pertinent Contributions in Toxicology Research >Recombinant paraoxonase 1 protects against sarin and soman toxicity following microinstillation inhalation exposure in guinea pigs.
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Recombinant paraoxonase 1 protects against sarin and soman toxicity following microinstillation inhalation exposure in guinea pigs.

机译:重组对氧磷酶1可防止豚鼠吸入微滴剂后沙林和梭曼的毒性。

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摘要

To explore the efficacy of paraoxonase 1 (PON1) as a catalytic bioscavenger, we evaluated human recombinant PON1 (rePON1) expressed in Trichoplusia ni larvae against sarin and soman toxicity using microinstillation inhalation exposure in guinea pigs. Animals were pretreated intravenously with catalytically active rePON1, followed by exposure to 1.2 X LCt sarin or soman. Administration of 5 units of rePON1 showed mild increase in the blood activity of the enzyme after 30 min, but protected the animals with a significant increase in survival rate along with minimal signs of nerve agent toxicity. Recombinant PON1 pretreated animals exposed to sarin or soman prevented the reduction of blood O saturation and pulse rate observed after nerve agent exposure. In addition, rePON1 pretreated animals showed significantly higher blood PON1, acetylcholinesterase (AChE), and butyrylcholinesterase activity after nerve agent exposure compared to the respective controls without treatments. AChE activity in different brain regions of rePON1 pretreated animals exposed to sarin or soman were also significantly higher than respective controls. The remaining activity of blood PON1, cholinesterases and brain AChE in PON1 pretreated animals after nerve agent exposure correlated with the survival rate. In summary, these data suggest that human rePON1 protects against sarin and soman exposure in guinea pigs.
机译:为了探索对氧磷酶1(PON1)作为催化生物清除剂的功效,我们使用豚鼠的微滴吸入法评估了在毛癣菌幼虫中表达的人重组PON1(rePON1)对沙林和梭曼的毒性。用催化活性的rePON1对动物进行静脉内预处理,然后暴露于1.2 X LCt沙林或梭曼。施用5个单位的REPON1在30分钟后显示出该酶血液活性的轻度增加,但以显着增加的存活率以及最小程度的神经毒剂毒性迹象保护了动物。暴露于沙林或梭曼的重组PON1预处理动物阻止了神经毒剂暴露后观察到的血O饱和度降低和脉搏率降低。此外,与未经治疗的各个对照组相比,经rePON1预处理的动物在接触神经制剂后显示出较高的血液PON1,乙酰胆碱酯酶(AChE)和丁酰胆碱酯酶活性。在暴露于沙林或梭曼的rePON1预处理动物的不同脑区中,AChE活性也显着高于相应对照组。暴露于神经制剂的PON1预处理动物中血液PON1,胆碱酯酶和脑AChE的剩余活性与存活率相关。总而言之,这些数据表明人rePON1可以防止豚鼠的沙林和梭曼暴露。

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