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Nitrite therapy improves survival postexposure to chlorine gas

机译:亚硝酸盐治疗改善了氯气的生存后曝光

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Exposure to relatively high levels of chlorine (Cl2) gas can occur in mass-casualty scenarios associated with accidental or intentional release. Recent studies have shown a significant postexposure injury phase to the airways, pulmonary, and systemic vasculatures mediated in part by oxidative stress, inflammation, and dysfunction in endogenous nitric oxide homeostasis pathways. However, there is a need for therapeutics that are amenable to rapid and easy administration in the field and that display efficacy toward toxicity after chlorine exposure. In this study, we tested whether nitric oxide repletion using nitrite, by intramuscular injection after CI2 exposure, could prevent CI2 gas toxicity. C57bl/6 male mice were exposed to 600 parts per million Cl2 gas for 45 min, and 24-h survival was determined with or without postexposure intramuscular nitrite injection. A single injection of nitrite (10 mg/kg) administered either 30 or 60 min postexposure significantly improved 24-h survival (from —20% to 50%). Survival was associated with decreased neutrophil accumulation in the airways. Rendering mice neutropenic before CI2 exposure improved survival and resulted in loss of nitrite-dependent survival protection. Interestingly, female mice were more sensitive to Cl2-induced toxicity compared with males and were also less responsive to postexposure nitrite therapy. These data provide evidence for efficacy and define therapeutic parameters for a single intramuscular injection of nitrite as a therapeutic after Cl2 gas exposure that is amenable to administration in mass-casualty scenarios.
机译:暴露于相对高水平的氯(Cl2)气体可能发生在与意外或有意释放相关的大规模伤亡场景中。最近的研究已经显示出在内源性一氧化氮稳态途径的氧化应激,炎症和功能障碍中介导的呼吸道,肺和全身血管的显着曝光损伤阶段。然而,需要治疗方法,其可在现场迅速轻松地施用,并且在氯暴露后显示毒性的疗效。在这项研究中,我们测试了在CI2暴露后通过肌肉注射的使用亚硝酸盐的一氧化氮补充,可以预防CI2气体毒性。将C57BL / 6雄性小鼠暴露于每百万份CL2气体45分钟45分钟,并测定24-H存活,或者没有颗粒肌肉内亚硝酸盐注射测定。单一注射亚硝酸盐(10mg / kg)30或60分钟后曝光明显改善了24-h生存(从-20%至50%)。存活与气道中的中性粒细胞积聚降低有关。在CI2曝光之前渲染小鼠中性腺增强的存活率,导致含氮酸盐依赖性的存活保护。有趣的是,与雄性相比,雌性小鼠对Cl2诱导的毒性更敏感,并且对胚胎亚硝酸盐治疗的响应也不太敏感。这些数据提供了有效性的证据,并定义了在CL2气体暴露后作为治疗性的单一肌肉注射亚颗粒的治疗参数,其可用于在大规模伤亡场景中给药。

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