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C5a在脓毒症多器官功能衰竭中的作用。

Role of C5a in multiorgan failure during sepsis.

作者信息

Huber-Lang M, Sarma V J, Lu K T, McGuire S R, Padgaonkar V A, Guo R F, Younkin E M, Kunkel R G, Ding J, Erickson R, Curnutte J T, Ward P A

机构信息

Department of Pathology University of Michigan Medical School, Ann Arbor, MI 48109, USA.

出版信息

J Immunol. 2001 Jan 15;166(2):1193-9. doi: 10.4049/jimmunol.166.2.1193.

Abstract

In humans with sepsis, the onset of multiorgan failure (MOF), especially involving liver, lungs, and kidneys, is a well known complication that is associated with a high mortality rate. Our previous studies with the cecal ligation/puncture (CLP) model of sepsis in rats have revealed a C5a-induced defect in the respiratory burst of neutrophils. In the current CLP studies, MOF occurred during the first 48 h with development of liver dysfunction and pulmonary dysfunction (falling arterial partial pressure of O(2), rising partial pressure of CO(2)). In this model an early respiratory alkalosis developed, followed by a metabolic acidosis with increased levels of blood lactate. During these events, blood neutrophils lost their chemotactic responsiveness both to C5a and to the bacterial chemotaxin, fMLP. Neutrophil dysfunction was associated with virtually complete loss in binding of C5a, but binding of fMLP remained normal. If CLP animals were treated with anti-C5a, indicators of MOF and lactate acidosis were greatly attenuated. Under the same conditions, C5a binding to blood neutrophils remained intact; in tandem, in vitro chemotactic responses to C5a and fMLP were retained. These data suggest that, in the CLP model of sepsis, treatment with anti-C5a prevents development of MOF and the accompanying onset of blood neutrophil dysfunction. This may explain the protective effects of anti-C5a in the CLP model of sepsis.

摘要

在患有脓毒症的人类中,多器官功能衰竭(MOF)的发生,尤其是涉及肝脏、肺和肾脏的多器官功能衰竭,是一种众所周知的并发症,与高死亡率相关。我们之前对大鼠脓毒症盲肠结扎/穿刺(CLP)模型的研究揭示了C5a诱导的中性粒细胞呼吸爆发缺陷。在当前的CLP研究中,MOF在最初的48小时内发生,同时出现肝功能障碍和肺功能障碍(动脉血氧分压下降,二氧化碳分压上升)。在这个模型中,早期出现呼吸性碱中毒,随后是代谢性酸中毒,血乳酸水平升高。在这些事件中,血液中的中性粒细胞对C5a和细菌趋化因子fMLP的趋化反应性丧失。中性粒细胞功能障碍实际上与C5a结合的完全丧失有关,但fMLP的结合仍保持正常。如果用抗C5a治疗CLP动物,MOF和乳酸酸中毒的指标会大大减轻。在相同条件下,C5a与血液中性粒细胞的结合保持完整;同时,对C5a和fMLP的体外趋化反应得以保留。这些数据表明,在脓毒症的CLP模型中,用抗C5a治疗可预防MOF的发生以及随之而来的血液中性粒细胞功能障碍。这可能解释了抗C5a在脓毒症CLP模型中的保护作用。

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