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首页> 外文期刊>Resuscitation. >Effect of speed of rewarming and administration of anti-inflammatory or anti-oxidant agents on acute lung injury in an intestinal ischemia model treated with therapeutic hypothermia.
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Effect of speed of rewarming and administration of anti-inflammatory or anti-oxidant agents on acute lung injury in an intestinal ischemia model treated with therapeutic hypothermia.

机译:在治疗性体温过低治疗的肠缺血模型中,复温速度和抗炎药或抗氧化剂的给药对急性肺损伤的影响。

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AIM OF THE STUDY: Acute lung injury (ALI) develops in various clinical situations and is associated with high morbidity and mortality and therapeutic hypothermia (HT) has been studied to attenuate the ALI. However, the optimal method of rewarming has not been determined. We determined the effect of speed of rewarming and the administration of anti-inflammatory or anti-oxidant agents on ALI in an intestinal ischemia and reperfusion (I/R) model treated with HT. MATERIALS AND METHODS: A Sprague-Dawley rat model of intestine ischemia and reperfusion was used. Two parallel animal experiments were conducted. In the survival study, rats (n=5 per group) underwent normothermic intestinal ischemia (60min, 36-38 degrees C) and then randomized into 7 groups with reperfusion: normothermia (NT), HT without rewarming (30-32 degrees C, HT), 2h HT+rewarming for 1h (RW1), 2h HT+rewarming for 2h (RW2), RW1+N-acetyl cysteine (RW-NAC), RW1+ethylpyruvate (RW-EP), and RW1+dexamethasone (RW+Dexa). In the second experiment, we investigated the histological and biochemical effects on the lung 4h after reperfusion (n=8 per group). RESULTS: The survival rate was lowest after NT. The HT, RW2, and RW-Dexa groups survived longer than the RW1, RW-NAC, and RW-EP groups. ALI scores were lower in the HT, RW2, and RW-Dexa groups than RW1. Lung malondialdehyde content was also lower in these groups. Interleukin (IL)-6 was significantly higher in the RW1 group. Inducible NO synthase gene expression in lung was lower in the HT, RW2, and RW-Dexa than RW1, and serum NO was lower in the RW2 and RW-Dexa than RW1. CONCLUSION: Gradual rewarming and administration of dexamethasone improved survival and attenuated ALI after intestinal I/R injury treated with HT in rats.
机译:研究目的:急性肺损伤(ALI)在各种临床情况下发展,并与高发病率和死亡率相关,并且已经研究了治疗性体温过低(HT)来减轻ALI。但是,尚未确定最佳的预热方法。我们确定了在用HT处理的肠道缺血和再灌注(I / R)模型中,热敏化速度和抗炎药或抗氧化剂对ALI的作用。材料与方法:采用Sprague-Dawley大鼠肠缺血再灌注模型。进行了两个平行的动物实验。在生存期研究中,大鼠(每组n = 5)经历了常温肠缺血(60分钟,36-38摄氏度),然后随机分为7组,进行了再灌注:常温(NT),HT无复温(30-32摄氏度, HT),2小时HT +重新武装1小时(RW1),2小时HT +重新武装2小时(RW2),RW1 + N-乙酰半胱氨酸(RW-NAC),RW1 +丙酮酸乙酯(RW-EP)和RW1 +地塞米松(RW + Dexa)。在第二个实验中,我们研究了再灌注后4h对肺的组织学和生化作用(每组n = 8)。结果:NT后生存率最低。 HT,RW2和RW-Dexa组的生存时间比RW1,RW-NAC和RW-EP组更长。 HT,RW2和RW-Dexa组的ALI得分低于RW1。这些组中肺丙二醛含量也较低。 RW1组中白介素(IL)-6明显更高。 HT,RW2和RW-Dexa中肺中可诱导的NO合酶基因表达低于RW1,而RW2和RW-Dexa中血清中NO低于RW1。结论:地塞米松逐渐加温和给药可提高大鼠肠I / R损伤后的存活率,并减轻ALI。

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