粒细胞集落刺激因子预防性治疗可改善出血和脓毒症双打击模型中的生存率并减轻炎症反应。

Granulocyte colony-stimulating factor prophylaxis improves survival and inflammation in a two-hit model of hemorrhage and sepsis.

作者信息

Bauhofer Artur, Lorenz Wilfried, Kohlert Frank, Torossian Alexander

机构信息

Institute of Theoretical Surgery, Philipps-University Marburg, Germany.

出版信息

Crit Care Med. 2006 Mar;34(3):778-84. doi: 10.1097/01.ccm.0000201900.01000.6b.

DOI:10.1097/01.ccm.0000201900.01000.6b

PMID:16521271

Abstract

OBJECTIVE

We evaluated the effects of a granulocyte-colony stimulating factor (G-CSF) prophylaxis in two clinically relevant situations, hemorrhage on the day before infection (e.g., trauma) and acute hemorrhage followed subsequently by infection (e.g., operative complication). A two-hit model of hemorrhage and polymicrobial peritoneal contamination and infection (PCI) was used to assess the influence of G-CSF on the outcome, bacterial clearance, and cytokine pattern.

DESIGN

Clinic modeling randomized laboratory trial.

SETTING

University laboratory.

SUBJECTS

One hundred thirty-two male rats.

INTERVENTIONS

In trial 1 we compared a) preoperative PCI only; b) preoperative hemorrhage plus PCI; and c) hemorrhage plus PCI plus G-CSF prophylaxis (n=18 rats/group). In trial 2, intraoperative hemorrhage was assessed with the same trial design. Primary end point was survival at 120 hrs. In trial 2 additionally, six rats per group and six naive control rats were used for secondary end point analysis.

MEASUREMENTS AND MAIN RESULTS

Primary end point was mortality at 120 hrs. Secondary end points were granulocyte counts, bacterial clearance, and local cytokine levels. In trial 1 survival rate was 56% after PCI only, 17% after hemorrhage plus PCI, and 61% after hemorrhage plus PCI plus G-CSF (p<.01). In trial 2 survival rate was 33% after PCI only, 17% after hemorrhage plus PCI, and 50% after hemorrhage plus PCI plus G-CSF (p<.05). In trial 2, neutrophil counts were doubled to 66% 1 hr after hemorrhage (p<.05), colony-forming units of microbes in the lung and liver were halved to 166+/-56 and 134+/-28 colony-forming units (p<.05 for liver), and the macrophage inflammatory protein-2 expression in the lung was halved to 0.88+/-0.06 pg of complementary DNA (p<.05) by G-CSF prophylaxis compared with hemorrhage and PCI.

CONCLUSIONS

Hemorrhage (first hit) sensitized the host for a second hit of polymicrobial PCI independent of the timing. G-CSF prophylaxis improved survival and clearance of microbes and reduced the proinflammatory chemokine macrophage inflammatory protein-2 in the lung.

摘要

目的

我们评估了粒细胞集落刺激因子（G-CSF）预防措施在两种临床相关情况下的效果，即感染前一天出血（如创伤）以及随后急性出血并继发感染（如手术并发症）。采用出血与多微生物腹腔污染及感染（PCI）的双打击模型来评估G-CSF对结局、细菌清除及细胞因子模式的影响。

设计

临床建模随机实验室试验。

地点

大学实验室。

研究对象

132只雄性大鼠。

干预措施

在试验1中，我们比较了：a）仅术前PCI；b）术前出血加PCI；c）出血加PCI加G-CSF预防（每组18只大鼠）。在试验2中，采用相同试验设计评估术中出血情况。主要终点为120小时时的生存率。在试验2中，每组另外选取6只大鼠及6只未处理的对照大鼠用于次要终点分析。

测量指标及主要结果

主要终点为120小时时的死亡率。次要终点为粒细胞计数、细菌清除及局部细胞因子水平。在试验1中，仅PCI后生存率为56%，出血加PCI后为17%，出血加PCI加G-CSF后为61%（p<0.01）。在试验2中，仅PCI后生存率为33%，出血加PCI后为17%，出血加PCI加G-CSF后为50%（p<0.05）。在试验2中，出血1小时后中性粒细胞计数增加一倍至66%（p<0.05），肺和肝脏中的微生物集落形成单位减半至166±56和134±28集落形成单位（肝脏p<0.05），与出血加PCI相比，G-CSF预防使肺中巨噬细胞炎性蛋白-2的表达减半至0.88±0.06 pg互补DNA（p<0.05）。