Effect of the position of the phenolic group in morphinans on their affinity for opiate receptor binding |
| |
Authors: | L D Simon F R Simon E Mohasci L Berger E J Simon |
| |
Institution: | 1. New York University Medical Center New York, N.Y. 10016, USA;7. Chemical Research Dept., Hoffmann-LaRoche, Inc., Nutley, N.J. 07110, USA |
| |
Abstract: | Homologous series of N-methyl, N-allyl and N-cyclopropylmethylmorphinans, differing only in the position of the plenolic hydroxy group, were examined with respect to their binding affinities for the opiate receptor. IC50's were determined for competition with 3H-naltrexone in the presence and absence of 100 mM NaCl. While the compounds with the hydroxy in the 3-position had, as expected, by far the highest affinity, the corresponding molecules with the hydroxy in the 2- or 4- position had significant binding affinity ranging from 30 nM in the cyclopropyl- methyl series to 400 nM for the 2-hydroxy N-methyl morphinan. The sodium indices were also very similar to those of the corresponding 3-hydroxy compounds. The only 1-hydroxy derivative available was about 5-fold weaker than the corresponding 2- and 4-hydroxy compounds. Covering or removing the hydroxy group greatly weakened the binding but did not totally destroy it. There was good correlation between binding affinity and pharmacological potency for all except the methoxy compounds. Their high potency is consonant with hydrolysis of the methyl ether. |
| |
Keywords: | |
本文献已被 ScienceDirect 等数据库收录! |
|