首页> 外文期刊>Japanese Journal of Pharmacology >Pharmacological Actions of the Racemic and the Enantiomeric 1, 4-Dimethyl-10-Hydroxy-2, 3, 4, 5, 6, 7-Hexahydro-1, 6-Methano-1H-4-Benzazonines (C-Homobenzomorphans)
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Pharmacological Actions of the Racemic and the Enantiomeric 1, 4-Dimethyl-10-Hydroxy-2, 3, 4, 5, 6, 7-Hexahydro-1, 6-Methano-1H-4-Benzazonines (C-Homobenzomorphans)

机译:外消旋和对映体1,4-二甲基-10-羟基-2,3,4,5,5,6,7-六氢-1,6-甲氧基-1H-4-苯并az子(C-Homobenzomorphans)的药理作用

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References(25) The racemate and optical isomers of the C-homobenzomorphans, 1, 4-dimethyl-10-hydroxy-2, 3, 4, 5, 6, 7-hexahydro-1, 6-methano-1H-4-benzazonine, were evaluated in a number of assays sensitive to narcotics of different types. All three C-homobenzomorphans were active in vitro in guinea pig ileum, mouse vas deferens, and rat brain membrane binding assays, but were of low potency. These C-homobenzomorphans showed different profiles of in vivo activity. The (+)-isomer and racemate were active as agonists in the tail-flick assay, whereas the (-)-isomer was inactive. At higher doses, the (-)-isomer and the racemate behaved as antagonists of morphine in the tail-flick assay. All three compounds were active in the phenylquinone test, but naloxone did not block this effect. In addition, all three were potent in the hot-plate test. Neither of the isomers substituted for morphine in dependent rats or monkeys. However, the (+)-isomer precipitated withdrawal in these monkeys. The (-)-isomer produced opioid-like physical dependence in both rats and monkeys. Some of the implications regarding the results with these remarkable homobenzomorphans are discussed.
机译:参考文献(25)C-高苯并吗啡酮的外消旋体和旋光异构体,1,4-二甲基-10-羟基-2,3,4,4,5,6,7-六氢-1,6-甲氨基-1H-4-苯并zon嗪在多种对不同类型麻醉品敏感的分析中进行了评估。在豚鼠回肠,小鼠输精管和大鼠脑膜结合试验中,所有三种C-高苯并吗啡酮均在体外具有活性,但效力较低。这些C-高苯并吗啡啉显示出不同的体内活性。在甩尾试验中,(+)-异构体和外消旋体是激动剂,而(-)-异构体则没有活性。在甩尾试验中,在较高剂量下,(-)-异构体和外消旋物可作为吗啡的拮抗剂。这三种化合物在苯醌测试中均具有活性,但纳洛酮并未阻止这种作用。另外,这三个在热板测试中均有效。在依赖的大鼠或猴子中,两种异构体均不能替代吗啡。然而,(+)-异构体在这些猴子中沉淀撤离。 (-)-异构体在大鼠和猴子中均产生类阿片样物质依赖性。讨论了有关这些显着的均苯并吗啡酮的结果的一些含义。

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