Lislott Eggstein-Aeppli scite author profile

Burkard²,

Eggstein-Aeppli³

et al. 1989

J. Med. Chem.

(-)-N-(Cyclopropylmethyl)-4,14-dimethoxymorphinan-6-one (2) was synthesized with 4,14-dimethoxy-N-methylmorphinan-6-one (1) as starting material. In vivo and in vitro experiments show 2 (cyprodime) to be a pure opioid receptor antagonist. Some of these tests (opioid receptor binding assays, guinea pig ileal longitudinal muscle preparation, rat and mouse vas deferens preparation, acetic acid writhing antagonism test) indicate that 2 is a selective mu opioid receptor antagonist.

Synthesis and Biological Evaluation of 14‐Alkoxymorphinans Part 4 opioid agonists and partial opioid agonists in a series of N‐(cyclobutylmethyl)‐14‐methoxymorphinan‐6‐ones

Burkard

Eggstein-Aeppli

1989

Helvetica Chimica Acta

(−)‐N‐[(Cyclopropyl) methyl]‐3,4‐dimethoxy‐5‐methylmorphinan‐6‐one, an opioid agonist with preference for kappa opioid receptors

Fritsch

Burkard

et al. 1988

Helvetica Chimica Acta

N-Allyl-and N-[(cyclopropyl)methyl]-3,4-dimethoxy-5-methylmorphinan-6-one (9 and 10, resp.) were synthesized from 5-methyldihydrothebainone (1). This essential intermediate was prepared from thebaine via 5-methylthebaine (5) employing a novel route. The pharmacological studies showed 9 and 10 to be potent opioid agonists. Compound 10 was found to have preference for kappa rather than mu opioid receptors.Introduction. -The opioid agonistic properties of N-methylmorphinan-6-ones are very much dependent on the substitution pattern at the aromatic ring [l]. Besides the 'natural' substitution pattern 3-hydroxy-4,5-epoxy, the 4-monomethoxy and the 3,4-dimethoxy substitution was found to be most effective. Among the compounds with high antinociceptive potency was 3,4-dimethoxy-5,17-dimethylrnorphinan-6-one (6) [2], which prompted us to replace its N-CH, group by substituents known to introduce in most cases opioid antagonistic effects in morphinans. We chose the N-ally1 and the N-(cyclopropy1)-methyl group which are present in the opioid antagonists naloxone and naltrexone, respectively.

An Opioid Agonist with Preference for κ‐Opioid Receptors: (−)‐N‐Cyclopropylmethylmorphinan‐6‐one

Trenker

Burkard

et al. 1990

Archiv der Pharmazie

ChemInform Abstract: (‐)‐N‐((Cyclopropyl)methyl)‐3,4‐dimethoxy‐5‐methylmorphinan‐6‐one an Opioid Agonist with Preference for Kappa Opioid Receptors.

et al. 1988