Department of Traumatology Semmelweis Medical University Peterfy Hospital P.O. Box 76 Budapest 1441 Hungary.
Mediators Inflamm. 1992;1(3):183-90. doi: 10.1155/S0962935192000280.
The effects of platelet activating factor (PAF) on eicosanoid release during endotoxic shock was investigated in anaesthetized pigs receiving 5 mug kg(-1) Escherichia coli endotoxin (LPS) into the superior mesenteric artery over a 60 min period, by measuring plasma levels of a variety of mediators. Fifteen of the 31 animals infused with LPS and not treated with BN 52021, a PAF receptor antagonist, died within 30 min after the commencement of LPS infusion (non-survivors), while the other 16 survived the experimental period of 3 h, though in a state of shock (survivors). No alterations were observed in plasma concentrations of eicosanoids in the non-survivors. A significant, though transient, increase in eicosanoid concentrations occurred only in the survivors. Treatment with BN 52021 (4 mg kg-1, i.v.) injected 5 min prior to LPS infusion, failed to exert any effect on the survival rate. However, pretreatment with BN 52021 prevented circulatory collapse in the survivors and reduced the concentration of cyclooxygenase enzyme products, without affecting LTB(4) release. Exogenous administration of PAF (0.01 mug kg(-1)) caused hypotension and increased TXB(2) levels although 6-keto PGF(1alpha) and LTB(4) concentrations were unchanged. The data suggest that prostanoid formation may be secondary to PAF release in circulatory collapse evoked by LPS infusion in survivors, and give further support to the suggestion that PAF prostanoid interaction is important during endotoxic shock. However, their role in early death seems to be negligible, indicating the importance of other mediators.
在麻醉猪中,通过测量各种介质的血浆水平,研究了血小板激活因子 (PAF) 在内毒素休克期间对花生四烯酸释放的影响。在 60 分钟内,将 5 微克/千克大肠杆菌内毒素(LPS)输注至上肠系膜动脉,其中 31 只动物中的 15 只未用 PAF 受体拮抗剂 BN 52021 治疗,在 LPS 输注开始后 30 分钟内死亡(非幸存者),而其余 16 只动物在 3 小时的实验期间存活,但处于休克状态(幸存者)。非幸存者的前列腺素水平没有变化。幸存者仅出现短暂的、显著的前列腺素浓度升高。在 LPS 输注前 5 分钟静脉注射 BN 52021(4 毫克/千克)治疗,对存活率没有影响。然而,BN 52021 的预处理可预防幸存者的循环衰竭,并降低环加氧酶酶产物的浓度,而不影响 LTB4 的释放。外源性给予 PAF(0.01 微克/千克)可引起低血压和 TXB2 水平升高,尽管 6-酮-PGF1alpha 和 LTB4 浓度不变。数据表明,在幸存者中由 LPS 输注引起的循环衰竭中,前列腺素的形成可能继发于 PAF 的释放,并进一步支持 PAF-前列腺素相互作用在内毒素休克中很重要的观点。然而,它们在早期死亡中的作用似乎可以忽略不计,这表明其他介质的重要性。