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一种选择性μ阿片受体激动剂和纳洛酮对氯化钠溶液摄入量的影响。

Effects of a selective mu opioid receptor agonist and naloxone on the intake of sodium chloride solutions.

作者信息

Gosnell B A, Majchrzak M J

机构信息

University of Michigan, Department of Psychiatry, Ann Arbor 48109-0116.

出版信息

Psychopharmacology (Berl). 1990;100(1):66-71. doi: 10.1007/BF02245792.

DOI:10.1007/BF02245792
PMID:2153308
Abstract

Endogenous opioid peptides are thought to play a role in mediating the palatability or rewarding aspects of sweet tastes. There is also evidence, however, which suggests that opioids may influence the preference for the taste of salt as well. In the present studies, we measured the effects of central administration of naloxone and the mu agonist [D-Ala2,MePhe4,Gly-ol5]enkephalin (DAGO) on the ingestion of salt solutions. In non-deprived rats given a choice of water and 0.6% saline, ICV injections of DAGO (1 and 3 nmol) significantly increased the intake of 0.6% saline; baseline water intake was minimal and was unaffected by DAGO. When rats were given a choice between water and 1.7% saline, DAGO stimulated both water and saline intake. Because 1.7% saline is a hypertonic solution, the increase in water intake may have been secondary to saline intake. In rats on a deprivation schedule in which water and 0.6% saline were available for only 2-3 h/day, there was a tendency for DAGO to increase 0.6% saline intake and decrease water intake, though these effects were not significant. In rats given water and 1.7% saline, DAGO increased saline intake and had no effect on water intake. Naloxone was also tested in water-deprived rats. Naloxone (20 and 50 micrograms) significantly decreased 0.6% saline intake; baseline water intake was low (3-5 ml) and was unaffected by naloxone. When rats were given a choice between water and 1.7% saline, naloxone (50 micrograms) significantly reduced water intake, while intake of 1.7% saline was slightly increased. These results suggest a role for central mu opioid receptors in mediating the preference for salt solutions.

摘要

内源性阿片肽被认为在介导甜味的适口性或奖赏性方面发挥作用。然而,也有证据表明阿片类物质可能同样会影响对盐味的偏好。在本研究中,我们测量了脑室内注射纳洛酮和μ激动剂[D - Ala2,MePhe4,Gly - ol5]脑啡肽(DAGO)对盐溶液摄入的影响。在非剥夺状态下可选择水和0.6%盐水的大鼠中,脑室内注射DAGO(1和3 nmol)显著增加了0.6%盐水的摄入量;基线水摄入量极少且不受DAGO影响。当大鼠在水和1.7%盐水之间进行选择时,DAGO刺激了水和盐水的摄入。由于1.7%盐水是高渗溶液,水摄入量的增加可能是盐水摄入的继发结果。在仅在每天2 - 3小时可获取水和0.6%盐水的剥夺方案下的大鼠中,DAGO有增加0.6%盐水摄入量并减少水摄入量的趋势,尽管这些影响并不显著。在给予水和1.7%盐水的大鼠中,DAGO增加了盐水摄入量且对水摄入量无影响。纳洛酮也在缺水大鼠中进行了测试。纳洛酮(20和50微克)显著降低了0.6%盐水的摄入量;基线水摄入量较低(3 - 5毫升)且不受纳洛酮影响。当大鼠在水和1.7%盐水之间进行选择时,纳洛酮(50微克)显著减少了水摄入量,而1.7%盐水的摄入量略有增加。这些结果表明中枢μ阿片受体在介导对盐溶液的偏好中发挥作用。

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本文引用的文献

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