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在清醒犬中,MIF-1在拮抗亮氨酸脑啡肽的心血管活性方面并不像纳洛酮那样起作用。

MIF-1 does not act like naloxone in antagonizing the cardiovascular activity of leucine-enkephalin in the conscious dog.

作者信息

Sander G E, Kastin A J, Giles T D

出版信息

Pharmacol Biochem Behav. 1982 Dec;17(6):1301-3. doi: 10.1016/0091-3057(82)90139-3.

Abstract

MIF-1 (Pro-Leu-Gly-NH2), a hypothalamic tripeptide, has been demonstrated to stimulate naloxone in antagonizing the effects of opioid peptides in a number of experimental systems including enkephalin-induced analgesia in the tail-flick assay, beta-endorphin induced hypothermia and hypomotility, deprivation-induced drinking, and analgesia in goldfish. MIF-1, however, has no effect upon the activity of enkephalins in the mouse vas deferens or enkephalin binding in the rat striatum. We have studied the interactions of MIF-1 with Leu5-enkephalin (Leu5-ENK) in the conscious, chronically instrumented dog. Although naloxone inhibits both the elevations of heart rate and blood pressure produced by IV Leu5-ENK in the conscious state and the depressions in these variables produced by Leu5-ENK after pentobarbital anesthesia, MIF-1 has no effect upon the Leu5-ENK response in either state. However, both naloxone and MIF-1 seem to raise mean arterial pressure in the conscious dog. These results indicate that MIF-1 does not act like naloxone in antagonizing the peripheral effects of Leu5-ENK and lend further support to the existence of mechanistic differences among opiate-mediated behavior, analgesia, and cardiovascular activity.

摘要

促黑素细胞激素释放抑制因子-1(脯氨酸-亮氨酸-甘氨酸-酰胺),一种下丘脑三肽,已证实在包括甩尾试验中脑啡肽诱导的镇痛、β-内啡肽诱导的体温过低和运动减少、剥夺诱导的饮水以及金鱼镇痛等多种实验系统中,它能刺激纳洛酮拮抗阿片肽的作用。然而,促黑素细胞激素释放抑制因子-1对小鼠输精管中脑啡肽的活性或大鼠纹状体中脑啡肽的结合没有影响。我们研究了促黑素细胞激素释放抑制因子-1与亮氨酸脑啡肽(亮氨酸脑啡肽)在清醒、长期植入仪器的犬中的相互作用。尽管纳洛酮在清醒状态下抑制静脉注射亮氨酸脑啡肽引起的心率和血压升高,以及戊巴比妥麻醉后亮氨酸脑啡肽引起的这些变量降低,但促黑素细胞激素释放抑制因子-1在这两种状态下对亮氨酸脑啡肽的反应均无影响。然而,纳洛酮和促黑素细胞激素释放抑制因子-1似乎都会使清醒犬的平均动脉压升高。这些结果表明,促黑素细胞激素释放抑制因子-1在拮抗亮氨酸脑啡肽的外周作用方面不像纳洛酮那样起作用,并进一步支持了阿片介导的行为、镇痛和心血管活动之间存在机制差异。

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