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Characterization of a model of systemic inflammation in humans in vivo elicited by continuous infusion of endotoxin

机译:通过连续输注内毒素引发体内体内全身炎症模型的特征

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摘要

Investigating the systemic inflammatory response in patients with critical illness such as sepsis, trauma and burns is complicated due to uncertainties about the onset, duration and severity of the insult. Therefore, in vivo models of inflammation are essential to study the pathophysiology and to evaluate immunomodulatory therapies. Intravenous bolus administration of endotoxin to healthy volunteers is a well-established model of a short-lived systemic inflammatory response, characterized by increased plasma cytokine levels, flu-like symptoms and fever. In contrast, patients suffering from systemic inflammation are often exposed to inflammatory stimuli for an extended period of time. Therefore, continuous infusion of endotoxin may better reflect the kinetics of the inflammatory response encountered in these patients. Herein, we characterize a novel model of systemic inflammation elicited by a bolus infusion of 1?ng/kg, followed by a 3hr continuous infusion of 1?ng/kg/h of endotoxin in healthy volunteers, and compared it with models of bolus administrations of 1 and 2?ng/kg of endotoxin. The novel model was well-tolerated and resulted in a more pronounced increase in plasma cytokine levels with different kinetics and more prolonged symptoms and fever compared with the bolus-only models. Therefore, the continuous endotoxin infusion model provides novel insights into kinetics of the inflammatory response during continuous inflammatory stimuli and accommodates a larger time window to evaluate immunomodulating therapies.
机译:由于对侮辱的发病,持续时间和严重程度的不确定性,调查患有疾病,创伤和烧伤等患者的全身炎症反应是复杂的。因此,在体内炎症模型对于研究病理生理学并评估免疫调节治疗至关重要。静脉注射血管诱导内毒素给健康的志愿者是一种良好的短期系统炎症反应模型,其特征在于血浆细胞因子水平增加,流感样症状和发烧。相比之下,患有全身炎症的患者通常在延长的一段时间内暴露于炎症刺激。因此,连续输注内毒素可以更好地反映这些患者遇到的炎症反应的动力学。在此,我们表征了通过1μg/ kg的推注输注引起的全身炎症的新型模型,然后在健康志愿者中进行3小时连续输注1μg/ kg / h的内毒素,并将其与推注施用的模型进行比较1和2?ng / kg内毒素。新型模型具有良好的耐受性,导致血浆细胞因子水平与不同动力学和更长的症状和发热的血浆细胞因子水平更加明显,与仅限推注模型相比。因此,连续内毒素输注模型为连续炎症刺激期间炎症反应的动力学提供了新的洞察力,并适应较大的时间窗口以评估免疫调节疗法。

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