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μ和κ阿片样物质激动剂对正常体温和冬眠地松鼠海马及下丘脑切片中5-羟色胺释放的调节作用。

The modulatory effects of mu and kappa opioid agonists on 5-HT release from hippocampal and hypothalamic slices of euthermic and hibernating ground squirrels.

作者信息

Cui Y, Lee T F, Kramarova L I, Wang L C

机构信息

Department of Zoology, University of Alberta, Edmonton, Canada.

出版信息

Life Sci. 1993;53(26):1957-65. doi: 10.1016/0024-3205(93)90017-w.

DOI:10.1016/0024-3205(93)90017-w
PMID:8255158
Abstract

To elucidate the role of opioids in regulating hibernation, the modulatory effects of different opioids on 35 mM K(+)-stimulated [3H]-5-HT release from brain slices were examined in the Richardson's ground squirrels. DAGO ([D-Ala2,N-Me-Phe4,Gly-ol5]-enkephalin), a specific mu agonist, evoked a significant dose-dependent (10(-7)-10(-5) M) inhibition of K(+)-stimulated 5-HT release from hippocampal slices of the non-hibernating squirrels. The inhibitory effect of DAGO was attenuated by either the opioid antagonist naloxone (10(-6) M) or the voltage dependent sodium channel blocker tetrodotoxin (TTX, 10(-6) M). The inhibitory effect of DAGO persisted in the hibernating squirrels; however, a ten fold higher concentration of DAGO (10(-6)-10(-5) M) was required to elicit a significant inhibition. In contrast, kappa agonist U50488 (10(-5) M) exerted a significant enhancement of K(+)-stimulated 5-HT release from hippocampal slices of the non-hibernating squirrels. This enhancement was blocked by either the specific kappa antagonist nor-binaltorphimine (10(-6) M) or TTX (10(-6) M). However, in the hibernating squirrels, the stimulatory effect of U50488 (10(-5) M) on 5-HT release was absent. DAGO and U50488 had no modulatory effects on K(+)-stimulated 5-HT release from the hypothalamic slices of either the non-hibernating or hibernating squirrels. These results demonstrate that the modulatory effects of opioids on 5-HT release are receptor-specific and state-dependent, indicating the complex nature of the roles of different opioids in regulating hibernation.

摘要

为阐明阿片类药物在调节冬眠中的作用,研究人员在理查森地松鼠中检测了不同阿片类药物对35 mM K(+)刺激的脑片[3H]-5-羟色胺(5-HT)释放的调节作用。特异性μ激动剂DAGO([D-Ala2,N-Me-Phe4,Gly-ol5]-脑啡肽)引起非冬眠松鼠海马切片中K(+)刺激的5-HT释放显著的剂量依赖性(10(-7)-10(-5) M)抑制。DAGO的抑制作用被阿片类拮抗剂纳洛酮(10(-6) M)或电压依赖性钠通道阻滞剂河豚毒素(TTX,10(-6) M)减弱。DAGO的抑制作用在冬眠松鼠中持续存在;然而,需要高10倍的DAGO浓度(10(-6)-10(-5) M)才能引起显著抑制。相比之下,κ激动剂U50488(10(-5) M)显著增强了非冬眠松鼠海马切片中K(+)刺激的5-HT释放。这种增强被特异性κ拮抗剂去甲二氢吗啡酮(10(-6) M)或TTX(10(-6) M)阻断。然而,在冬眠松鼠中不存在U(50488)(10(-5) M)对5-HT释放的刺激作用。DAGO和U50488对非冬眠或冬眠松鼠下丘脑切片中K(+)刺激的5-HT释放均无调节作用。这些结果表明,阿片类药物对5-HT释放的调节作用具有受体特异性和状态依赖性,表明不同阿片类药物在调节冬眠中的作用具有复杂性。

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