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酒精性肝炎合并肝硬化时的中性粒细胞功能障碍是可逆的,且可预测预后。

Neutrophil dysfunction in alcoholic hepatitis superimposed on cirrhosis is reversible and predicts the outcome.

作者信息

Mookerjee Rajeshwar P, Stadlbauer Vanessa, Lidder Sukhwinderjit, Wright Gavin A K, Hodges Stephen J, Davies Nathan A, Jalan Rajiv

机构信息

Liver Failure Group, Institute of Hepatology, Division of Medicine, University College London, London, UK.

出版信息

Hepatology. 2007 Sep;46(3):831-40. doi: 10.1002/hep.21737.

Abstract

UNLABELLED

Mortality in patients with alcoholic hepatitis (AH) remains high, and although corticosteroids are widely used for treatment, the results vary considerably. In AH, neutrophils are primed and infiltrate the liver to produce injury, but paradoxically, the main cause of death in such patients is infection. Our prospective study addressed this paradox of primed neutrophils on the one hand and increased risk of infection on the other. We hypothesized that the full activation of neutrophils by a humoral factor such as endotoxin renders them unable to respond to further bacterial challenge. We analyzed neutrophil oxidative burst and phagocytosis in whole blood by fluorescence-activated cell sorting analysis in 63 alcoholic patients with cirrhosis and patients with cirrhosis with superimposed AH (cirrhosis+AH). In 16 patients, ex vivo studies determined whether the removal of endotoxin restored neutrophil function. A resting burst greater than or equal to 55[corrected]%, indicating neutrophil activation and a reduced phagocytic capacity lower than 42%, was associated with significantly greater risk of infection, organ failure, and mortality. This defective neutrophil function was transmissible through patients' plasma to normal neutrophils, and patients' neutrophil function could be restored by normal plasma. The ex vivo removal of endotoxin from patients' plasma decreased the resting burst and increased the phagocytic function.

CONCLUSIONS

Our study provides the rationale for a goal-directed approach to the management of patients with cirrhosis and AH, in which the assessment of neutrophil function may be an important biomarker to select patients for immunosuppressive therapy. The neutrophil dysfunction in cirrhosis and AH is reversible, with endotoxin-removal strategies providing new targets for intervention.

摘要

未标注

酒精性肝炎(AH)患者的死亡率仍然很高,尽管皮质类固醇被广泛用于治疗,但其结果差异很大。在AH中,中性粒细胞被激活并浸润肝脏以造成损伤,但矛盾的是,这类患者的主要死因是感染。我们的前瞻性研究解决了一方面中性粒细胞被激活而另一方面感染风险增加这一矛盾。我们假设,诸如内毒素等体液因子对中性粒细胞的完全激活使其无法对进一步的细菌挑战作出反应。我们通过荧光激活细胞分选分析,对63例肝硬化酒精性患者以及肝硬化合并AH(肝硬化+AH)患者的全血中性粒细胞氧化爆发和吞噬作用进行了分析。在16例患者中,体外研究确定了内毒素的去除是否能恢复中性粒细胞功能。静息爆发大于或等于55[校正]%,表明中性粒细胞被激活,吞噬能力降低低于42%,这与感染、器官衰竭和死亡的风险显著增加相关。这种有缺陷的中性粒细胞功能可通过患者血浆传递给正常中性粒细胞,而患者的中性粒细胞功能可通过正常血浆恢复。从患者血浆中体外去除内毒素可降低静息爆发并增加吞噬功能。

结论

我们的研究为肝硬化和AH患者的目标导向管理方法提供了理论依据,其中中性粒细胞功能评估可能是选择免疫抑制治疗患者的重要生物标志物。肝硬化和AH中的中性粒细胞功能障碍是可逆的,内毒素去除策略提供了新的干预靶点。

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