morphinans and phenylbenzoquinone

morphinans has been researched along with phenylbenzoquinone* in 2 studies

Other Studies

2 other study(ies) available for morphinans and phenylbenzoquinone

Article	Year
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-benz azo nines (C-homobenzomorphans). Japanese journal of pharmacology, 1985, Volume: 39, Issue:1 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-benzaz onine, 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. Topics: Analgesics; Animals; Benzomorphans; Benzoquinones; Binding, Competitive; Body Weight; Etorphine; Guinea Pigs; In Vitro Techniques; Macaca mulatta; Male; Mice; Morphinans; Muscle Contraction; Muscle, Smooth; Quinones; Rats; Rats, Inbred Strains; Reaction Time; Stereoisomerism; Substance-Related Disorders	1985
9 alpha- and 9 beta-Hydroxyphenylmorphans. Journal of pharmaceutical sciences, 1984, Volume: 73, Issue:12 Platinum-oxide hydrogenation of 5-m-methoxyphenyl-2-methyl-9-oxomorphan (I) gave the 9 alpha-hydroxy racemate (II) whose phenolic analogue (III) is a strong antinociceptive agent, fully supportive of morphine dependence in rhesus monkeys. The di-O-acetyl derivative (VI) of III was similar to III in its profile of activity. The diastereoisomer of III (VII), obtained by hydrogenation of the methobromide of I (IV), extrusion of methyl bromide, and O-demethylation of the resultant free base (VIII), was almost inactive antinociceptively and did not suppress withdrawal symptoms in morphine-dependent monkeys. The orientation of the C-9 hydroxyl groups was deduced from spectral data and by analogy. Topics: Analgesics; Animals; Benzoquinones; Chemical Phenomena; Chemistry; Humans; Macaca mulatta; Mice; Morphinans; Pain; Quinones; Reaction Time; Stereoisomerism; Substance Withdrawal Syndrome	1984

Article

Year

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-benz azo nines (C-homobenzomorphans).

Japanese journal of pharmacology, 1985, Volume: 39, Issue:1

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-benzaz onine, 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.

Topics: Analgesics; Animals; Benzomorphans; Benzoquinones; Binding, Competitive; Body Weight; Etorphine; Guinea Pigs; In Vitro Techniques; Macaca mulatta; Male; Mice; Morphinans; Muscle Contraction; Muscle, Smooth; Quinones; Rats; Rats, Inbred Strains; Reaction Time; Stereoisomerism; Substance-Related Disorders

1985

9 alpha- and 9 beta-Hydroxyphenylmorphans.

Journal of pharmaceutical sciences, 1984, Volume: 73, Issue:12

Platinum-oxide hydrogenation of 5-m-methoxyphenyl-2-methyl-9-oxomorphan (I) gave the 9 alpha-hydroxy racemate (II) whose phenolic analogue (III) is a strong antinociceptive agent, fully supportive of morphine dependence in rhesus monkeys. The di-O-acetyl derivative (VI) of III was similar to III in its profile of activity. The diastereoisomer of III (VII), obtained by hydrogenation of the methobromide of I (IV), extrusion of methyl bromide, and O-demethylation of the resultant free base (VIII), was almost inactive antinociceptively and did not suppress withdrawal symptoms in morphine-dependent monkeys. The orientation of the C-9 hydroxyl groups was deduced from spectral data and by analogy.

Topics: Analgesics; Animals; Benzoquinones; Chemical Phenomena; Chemistry; Humans; Macaca mulatta; Mice; Morphinans; Pain; Quinones; Reaction Time; Stereoisomerism; Substance Withdrawal Syndrome

1984