Abstract
Early molecular modeling studies with Δ9-tetrahydrocannabinol (Δ9-THC) reported that three discrete regions which interact with brain cannabinoid (CB1) receptors corresponded to the C-9 position of the cyclohexene ring, the phenolic hydroxyl and the carbon side chain at the C3 position. Although the location of these attachment points for aminoalkylindoles is less clear, the naphthalene ring, the carbonyl group and the morpholinoethyl group have been suggested as probable sites. In this study, a series of indole- and pyrrole-derived cannabinoids was developed, in which the morpholinoethyl group was replaced with another cyclic structure or with a carbon chain that more directly corresponded to the side chain of Δ9-THC and were tested for CB1 binding affinity and in a battery of in vivo tests, including hypomobility, antinociception, hypothermia and catalepsy in mice and discriminative stimulus effects in rats. Receptor affinity and potency of these novel cannabinoids were related to the length of the carbon chain. Short side chains resulted in inactive compounds, whereas chains with 4 to 6 carbons produced optimal in vitro andin vivo activity. Pyrrole-derived cannabinoids were consistently less potent than were the corresponding indole derivatives and showed pronounced separation of activity, in that potencies for hypomobility and antinociception were severalfold higher than potencies for hypothermia and ring immobility. These results suggest that, whereas the site of the morpholinoethyl group in these cannabinoids seems crucial for attachment to CB1 receptors, the exact structural constraints on this part of the molecule are not as strict as previously thought.
Footnotes
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Send reprint requests to: Dr. Jenny L. Wiley, Department of Pharmacology and Toxicology, Medical College of Virginia, Virginia Commonwealth University, P.O. Box 980613, Richmond, VA 23298-0613.
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↵1 Research supported by National Institute on Drug Abuse Grants DA-03672 (B.R.M.) and DA-03590 (J.W.H.).
- Abbreviations:
- DD
- drug discrimination
- MPE
- maximal possible antinociceptive effect
- RI
- ring immobility
- RT
- rectal temperature
- SA
- spontaneous activity
- Δ9-THC
- Δ9-tetrahydrocannabinol
- BSA
- bovine serum albumin
- EDTA
- ethylenediaminetetraacetic acid
- Received December 16, 1997.
- Accepted February 13, 1998.
- The American Society for Pharmacology and Experimental Therapeutics
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