CBD-DMH
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Formula | C25H38O2 |
Molar mass | 370.577 g·mol−1 |
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Cannabidiol-dimethylheptyl (CBD-DMH or DMH-CBD) is a synthetic homologue of cannabidiol where the pentyl chain has been replaced by a dimethylheptyl chain. Several isomers of this compound are known. The most commonly used isomer in research is (−)-CBD-DMH, which has the same stereochemistry as natural cannabidiol, and a 1,1-dimethylheptyl side chain. This compound is not psychoactive and acts primarily as an anandamide reuptake inhibitor, but is more potent than cannabidiol as an anticonvulsant and has around the same potency as an antiinflammatory.[1][2][3][4] Unexpectedly the “unnatural” enantiomer (+)-CBD-DMH, which has reversed stereochemistry from cannabidiol, was found to be a directly acting cannabinoid receptor agonist with a Ki of 17.4nM at CB1 and 211nM at CB2, and produces typical cannabinoid effects in animal studies,[5] as does its 7-OH derivative.[6]
Another closely analogous compound has also been described, with the double bond in the cyclohexene ring shifted to between the 1,6-positions rather than the 2,3-positions (i.e. analogous to synthetic THC analogues such as parahexyl), the isopropenyl group saturated to isopropyl, and a 1,2-dimethylheptyl side chain. It is synthesized by Birch reduction from the 1,2-dimethylheptyl analogue of cannabidiol. This compound also produces potent cannabinoid-like effects in animals, but has three chiral centers and is composed of a mixture of eight stereoisomers, which have not been studied individually, so it is not known which stereoisomers are active.[7][8]
See also
- 7-OH-CBD
- Abnormal cannabidiol
- Cannabinoid receptors
- Cannabidiphorol
- Cis-THC
- HU-211
- HUF-101
- KLS-13019
- O-1656
- O-1871
- O-1918
- Nabilone
- Tetrahydrocannabiphorol
- NESS-040C5
References
- ^ Leite JR, Carlini EA, Lander N, Mechoulam R (1982). "Anticonvulsant effects of the (-) and (+)isomers of cannabidiol and their dimethylheptyl homologs". Pharmacology. 24 (3): 141–6. doi:10.1159/000137588. PMID 7071126.
- ^ Bisogno T, Hanus L, De Petrocellis L, Tchilibon S, Ponde DE, Brandi I, et al. (October 2001). "Molecular targets for cannabidiol and its synthetic analogues: effect on vanilloid VR1 receptors and on the cellular uptake and enzymatic hydrolysis of anandamide". British Journal of Pharmacology. 134 (4): 845–52. doi:10.1038/sj.bjp.0704327. PMC 1573017. PMID 11606325.
- ^ Ben-Shabat S, Hanus LO, Katzavian G, Gallily R (February 2006). "New cannabidiol derivatives: synthesis, binding to cannabinoid receptor, and evaluation of their antiinflammatory activity". Journal of Medicinal Chemistry. 49 (3): 1113–7. doi:10.1021/jm050709m. PMID 16451075.
- ^ Juknat A, Kozela E, Kaushansky N, Mechoulam R, Vogel Z (May 2016). "Anti-inflammatory effects of the cannabidiol derivative dimethylheptyl-cannabidiol - studies in BV-2 microglia and encephalitogenic T cells". Journal of Basic and Clinical Physiology and Pharmacology. 27 (3): 289–96. doi:10.1515/jbcpp-2015-0071. PMID 26540221.
- ^ Hanus LO, Tchilibon S, Ponde DE, Breuer A, Fride E, Mechoulam R (March 2005). "Enantiomeric cannabidiol derivatives: synthesis and binding to cannabinoid receptors". Organic & Biomolecular Chemistry. 3 (6): 1116–23. doi:10.1039/B416943C. PMID 15750656.
- ^ Fride E, Ponde D, Breuer A, Hanus L (June 2005). "Peripheral, but not central effects of cannabidiol derivatives: mediation by CB(1) and unidentified receptors". Neuropharmacology. 48 (8): 1117–29. doi:10.1016/j.neuropharm.2005.01.023. PMID 15910887. S2CID 16531395.
- ^ Razdan RK, Pars HG, Thompson WR, Granchelli FE (1974). "Lithium-ammonia reduction of tetrahydrocannabinols". Tetrahedron Letters. 15 (49–50): 4315–4318. doi:10.1016/S0040-4039(01)92152-5.
- ^ Razdan RK (1981). "The Total Synthesis of Cannabinoids". In Apsimon J (ed.). The Total Synthesis of Natural Products. Wiley Interscience. p. 245. ISBN 978-0-471-05460-3. OCLC 19487018.