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Oxygen and surgical site infection: a study of underlying immunologic mechanisms.

机译:氧气和手术部位感染:潜在的免疫机制研究。

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摘要

BACKGROUND: Recent clinical trials investigating the role of hyperoxia in decreasing surgical site infection have reported conflicting results. Immunologic mechanisms through which supplemental oxygen could act have not been elucidated fully. The authors sought to investigate the effects of hyperoxia on previously tested and prognostically significant innate immune parameters to uncover the potential effects of hyperoxia at the cellular level. METHODS: After formal approval and informed consent, venous blood samples were collected from young healthy volunteers. Corresponding samples were incubated at 21 or 80% O2 following a 1 ng/ml lipopolysaccharide challenge and analyzed to determine human leukocyte antigen-DR surface receptor expression, cytokine release, phagocytic capacity, and formation of reactive oxygen species. Data are presented as mean +/- SD. RESULTS: After the 2 h of incubation at 21% O2 (room air) and in 80% O2 chambers, the change in human leukocyte antigen-DR mean channel fluorescence in lipopolysaccharide-stimulated monocytes was 2,177 +/- 383 and 2,179 +/- 338 (P = 0.96), respectively. Tumor necrosis factor-alpha concentrations were significantly lower for samples incubated at 80% O2 when compared with 21% O2 (P < 0.05). The phagocytic capacity of the innate immune system was not significantly enhanced by supplemental oxygen. However, the formation of reactive oxygen species increased by 87% (P < 0.05). CONCLUSION: Hyperoxia exerts significant effects on multiple cellular and immunologic parameters, providing a potential mechanism for benefits from the use of supplemental oxygen. However, the ability to translate positive basic scientific findings to the operating suite or bedside require the existence of similar innate immune processes in vivo and the efficient transfer of oxygen to the sites where it may be used.
机译:背景:最近研究高氧在减少手术部位感染中作用的临床试验报告了相互矛盾的结果。尚不能完全阐明补充氧气可以通过其起作用的免疫机制。作者试图研究高氧对先前测试的和预后重要的先天免疫参数的影响,以揭示高氧在细胞水平上的潜在作用。方法:经过正式批准和知情同意后,从年轻健康志愿者那里采集静脉血样本。在1 ng / ml脂多糖激发后,将相应的样品在21%或80%的O2下孵育,并进行分析,以确定人白细胞抗原DR表面受体的表达,细胞因子的释放,吞噬能力和活性氧的形成。数据表示为平均值+/- SD。结果:在21%的氧气(室内空气)和80%的氧气室中孵育2小时后,脂多糖刺激的单核细胞中人白细胞抗原DR平均通道荧光的变化为2,177 +/- 383和2,179 +/-分别为338(P = 0.96)。与21%O2相比,在80%O2下孵育的样品的肿瘤坏死因子-α浓度明显更低(P <0.05)。补充氧气不能明显增强先天免疫系统的吞噬能力。但是,活性氧的形成增加了87%(P <0.05)。结论:高氧对多种细胞和免疫学参数具有显着影响,为补充氧气的使用提供了潜在的益处。然而,将阳性基础科学发现转化为手术室或床边的能力要求体内存在类似的先天免疫过程,并且需要将氧气有效转移到可以使用的部位。

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