在肝缺血-再灌注过程中,吞噬细胞激活活性氧产生,增强了内毒素诱导的肝损伤的易感性。

Circulatory shock Pub Date : 1994-05-01
P Liu, S L Vonderfecht, M A Fisher, G M McGuire, H Jaeschke
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引用次数: 0

摘要

在雄性Fischer大鼠肝缺血30分钟后再灌注4小时,监测血浆谷胱甘肽二硫(GSSG)水平,作为血管氧化应激、肿瘤坏死因子- α (tnf - α)形成和肝脏损伤(丙氨酸转氨酶活性、组织学)的指标。腹腔注射1 mg/kg肠炎沙门氏菌内毒素可增强缺血后氧化应激和肝损伤。缺血再灌注后,内毒素后tnf - α水平从10 +/- 7 pg/ml(基线)增加到3,553 +/- 738 pg/ml,或单独内毒素后增加到3,670 +/- 508 pg/ml。缺血前血清补体的消耗使内毒素介导的活性氧形成的增加减少了70%,但不影响tnf - α水平。眼镜蛇毒因子(CVF)在再灌注过程中的补体活化作用与内毒素对氧化应激和肝损伤的作用相似。CVF不增加再灌注时tnf - α的形成。注射内毒素2.5小时后,从缺血后肝脏分离的Kupffer细胞和中性粒细胞产生的超氧化物分别比从对照肝脏分离的细胞多600%和400%。结果表明,即使在短时间的肝缺血后,肝吞噬细胞也会大量启动活性氧产生,但不会形成tnf - α,并且肝缺血后易受内毒素诱导的严重损伤。活化补体似乎是产生这种效果的主要原因。这些结果可以解释广泛肝切除和低血容量性休克后肝功能衰竭的高风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Priming of phagocytes for reactive oxygen production during hepatic ischemia-reperfusion potentiates the susceptibility for endotoxin-induced liver injury.

Plasma levels of glutathione disulfide (GSSG) as an indicator of a vascular oxidant stress, tumor necrosis factor-alpha (TNF-alpha) formation, and liver injury (alanine aminotransferase activity, histology) were monitored in male Fischer rats after 30 min of hepatic ischemia followed by up to 4 hr of reperfusion. The injection of 1 mg/kg Salmonella enteritidis endotoxin at 30 min of reflow potentiated the postischemic oxidant stress and liver injury. TNF-alpha levels increased from 10 +/- 7 pg/ml (baseline) to 3,553 +/- 738 pg/ml after ischemia-reperfusion followed by endotoxin, or to 3,670 +/- 508 pg/ml after endotoxin alone. Depletion of serum complement before ischemia attenuated the endotoxin-mediated increase of reactive oxygen formation by 70% but did not affect TNF-alpha levels. Complement activation with cobra venom factor (CVF) during reperfusion had an effect similar to that of endotoxin on the oxidant stress and liver injury. CVF did not increase TNF-alpha formation during reperfusion. Kupffer cells and neutrophils isolated from the postischemic liver 2.5 hr after endotoxin injection generated 600% and 400% more superoxide, respectively, than cells isolated from control livers. The results demonstrate a substantial priming of hepatic phagocytes for reactive oxygen production but not TNF-alpha formation, even after short periods of hepatic ischemia, and the vulnerability of the postischemic liver to severe endotoxin-induced injury. Activated complement seems to be mainly responsible for the effects. These results may explain the high risk for hepatic failure after extensive liver resection and hypovolemic shock.

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