Systemic low-grade inflammation is recognized in an increasing number of chronic diseases. With the aim of establishing an experimental human in vivo model of systemic low-grade inflammation, we measured circulating inflammatory mediators after intravenous administration of Escherichia coli endotoxin (0.3 ng/kg of body weight) either as a bolus injection or as a 4-h continuous intravenous infusion, as well as after saline administration, in 10 healthy male subjects on three separate study days. Only bolus endotoxin caused an increase in heart rate, whereas a slight increase in rectal temperature was observed in both endotoxin groups. Tumor necrosis factor alpha (TNF-α), interleukin-6, and neutrophil responses were earlier and more pronounced in the bolus trial compared with the infusion trial results, whereas lymphocytes increased after endotoxin bolus injection as well as infusion without any difference between groups. Finally, endotoxin activated the hypothalamo-pituitary-adrenal axis slightly earlier in the bolus compared to the infusion trial. The continuous endotoxin infusion model may be more representative of human low-grade inflammation than the bolus injection model due to a less dynamic and more sustained increase in circulating levels of inflammatory mediators over time. In conclusion, low-dose endotoxin infusion elicits an inflammatory response, as assessed by a rise in TNF-α, and the responses are significantly different according to whether low-dose endotoxin is applied as a bolus injection or as a continuous infusion.
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机译:在越来越多的慢性疾病中已认识到全身性轻度炎症。为了建立实验性的人体体内系统性轻度炎症模型,我们在静脉内注射大肠埃希氏菌内毒素(0.3 ng / kg体重)或大剂量后,测量了循环炎症介质。在三个独立的研究日中,在10位健康的男性受试者中注射或进行4小时连续静脉输注以及在给予生理盐水后。在两个内毒素组中,仅推注内毒素引起心率增加,而观察到直肠温度略有升高。与推注试验结果相比,推注试验中肿瘤坏死因子α(TNF-α),白细胞介素6和中性粒细胞反应更早,更明显,而内毒素推注和输注后淋巴细胞增加,两组之间无任何差异。最后,与输液试验相比,内毒素在推注中稍早地激活了下丘脑-垂体-肾上腺轴。连续内毒素输注模型比快速浓注模型更能代表人的轻度炎症,因为随着时间的推移,炎症介质循环水平的动态性降低且持续性提高。总之,低剂量内毒素输注可引起炎症反应(如TNF-α升高所评估),并且根据是将大剂量内毒素用作大剂量注射还是连续输注而产生明显不同的反应。
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