首页> 外文期刊>The Journal of trauma >LF 16-0687 Ms, a new bradykinin B2 receptor antagonist, improves neurologic outcome but not brain tissue prostaglandin E2 release in a rat model of closed head trauma combined with ethanol intoxication.
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LF 16-0687 Ms, a new bradykinin B2 receptor antagonist, improves neurologic outcome but not brain tissue prostaglandin E2 release in a rat model of closed head trauma combined with ethanol intoxication.

机译:LF 16-0687 Ms是一种新型缓激肽B2受体拮抗剂,在闭合性颅脑外伤并伴有乙醇中毒的大鼠模型中,可改善神经功能,但不能改善脑组织前列腺素E2的释放。

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BACKGROUND: LF 16-0687 Ms previously was reported to improve Neurological Severity Score (NSS) and decrease cerebral edema and prostaglandin E(2) (PGE(2)) release after closed head trauma (CHT) in rats. Here, we examined whether these beneficial effects of LF 16-0687 Ms are altered when CHT is accompanied by acute ethanol administration. METHODS: Six groups of rats (n = 8 per group) were examined during combination of the following experimental conditions: CHT versus sham operation, LF 16-0687 Ms 3 mg/kg subcutaneously versus saline, and ethanol 2 g/kg versus saline. RESULTS: After CHT, brain water content decreased and NSS improved with ethanol + LF 16-0687 Ms as compared with values after saline or ethanol. PGE(2) release decreased with ethanol (147 +/- 59 pg/mg tissue) but not with ethanol + LF 16-0687 Ms (286 +/- 194 pg/mg tissue). CONCLUSION: Ethanol does not affect the improvement of NSS and the decrease of cerebral edema seen with LF 16-0687 Ms after CHT, but does reverse the ability of LF 16-0687 Ms to minimize the increase of PGE(2) release. In intoxicated patients, bradykinin antagonist therapy may improve post-CHT outcome without altering PGE(2) release.
机译:背景:以前曾报道LF 16-0687 Ms可改善大鼠闭合性颅脑创伤(CHT)后的神经系统严重程度评分(NSS),并降低脑水肿和前列腺素E(2)(PGE(2))的释放。在这里,我们检查了CHT伴随急性乙醇给药时,LF 16-0687 Ms的这些有益作用是否被改变。方法:在以下实验条件的组合下检查了六组大鼠(每组n = 8):CHT与假手术,LF 16-0687 Ms 3 mg / kg皮下注射生理盐水,2 g / kg乙醇注射生理盐水。结果:与盐水或乙醇处理相比,CHT处理后,乙醇+ LF 16-0687 Ms处理后脑水含量降低,NSS改善。 PGE(2)释放在乙醇(147 +/- 59 pg / mg组织)下降低,但在乙醇+ LF 16-0687 Ms(286 +/- 194 pg / mg组织)下没有降低。结论:乙醇不会影响CHT后LF 16-0687 Ms引起的NSS改善和脑水肿的减少,但会逆转LF 16-0687 Ms最小化PGE(2)释放增加的能力。在中毒的患者中,缓激肽拮抗剂治疗可改善CHT后的预后而不改变PGE(2)的释放。

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