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β-内啡肽:对人类的镇痛和激素作用。

beta-Endorphin: analgesic and hormonal effects in humans.

作者信息

Foley K M, Kourides I A, Inturrisi C E, Kaiko R F, Zaroulis C G, Posner J B, Houde R W, Li C H

出版信息

Proc Natl Acad Sci U S A. 1979 Oct;76(10):5377-81. doi: 10.1073/pnas.76.10.5377.

Abstract

The pharmacokinetics and the hormonal, analgesic, and behavioral effects of several doses of human beta-endorphin were evaluated after intravenous administration to three patients and intracerebroventricular administration to one patient with pain caused by cancer. These effects were compared to the hormonal effects of intravenously administered morphine sulfate in two patients and an enkephalin analog in two baboons. The mean terminal half-life after intravenous administration of 5 or 10 mg of human beta-endorphin to three patients was 37 min; the mean volume of distribution was 178 ml/kg, and the metabolic clearance rate was 3.2 (ml/min)/kg. The half-life of beta-endorphin in cerebrospinal fluid after intracerebroventricular administration was 93 min, and the volume of distribution was 0.74 ml/kg. A rapid rise in plasma prolactin followed both intravenous and intracerebroventricular beta-endorphin. Intravenous administration did not affect plasma growth hormone, but intracerebroventricular administration suppressed plasma growth hormone. No significant change in plasma growth hormone was noted after intravenous administration of morphine to humans, but plasma growth hormone decreased in one baboon after administration of the enkephalin analog. beta-Endorphin-stimulated release of prolactin occurred at doses lower than those required to produce analgesic and other behavioral effects. When both hormonal and analgesic effects were observed (after 7.5 mg were given intracerebroventricularly), the onset of the hormonal response slightly preceded the analgesic and behavioral responses. These studies suggest that the hormonal effects of beta-endorphin are species dependent and are similar to those of morphine. Hormonal and analgesic effects of beta-endorphin appear to result from the activation of opiate receptors that differ in their locations and characteristics.

摘要

对三名患者静脉注射以及对一名因癌症疼痛的患者脑室内注射多剂量人β-内啡肽后,评估了其人β-内啡肽的药代动力学以及激素、镇痛和行为效应。将这些效应与两名患者静脉注射硫酸吗啡以及两只狒狒静脉注射脑啡肽类似物的激素效应进行了比较。对三名患者静脉注射5或10毫克人β-内啡肽后的平均终末半衰期为37分钟;平均分布容积为178毫升/千克,代谢清除率为3.2(毫升/分钟)/千克。脑室内注射后β-内啡肽在脑脊液中的半衰期为93分钟,分布容积为0.74毫升/千克。静脉注射和脑室内注射β-内啡肽后血浆催乳素均迅速升高。静脉注射不影响血浆生长激素,但脑室内注射会抑制血浆生长激素。对人静脉注射吗啡后血浆生长激素无显著变化,但对一只狒狒注射脑啡肽类似物后血浆生长激素降低。β-内啡肽刺激催乳素释放的剂量低于产生镇痛和其他行为效应所需的剂量。当观察到激素和镇痛效应时(脑室内注射7.5毫克后),激素反应的开始略早于镇痛和行为反应。这些研究表明,β-内啡肽的激素效应具有物种依赖性,且与吗啡的效应相似。β-内啡肽的激素和镇痛效应似乎是由位置和特性不同的阿片受体激活所致。

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