2016 Mar 30;116:252-266. doi: 10.1016/j.ejmech.2016.03.072.
[Epub ahead of print]
Abstract
Targeting type-2 cannabinoid receptor (CB2) is considered a feasible strategy to develop new drugs for the treatment of diseases like neuropathic pain, chronic inflammation, neurodegenerative disorders and cancer. Such drugs are devoid of the undesired central side effects that are typically mediated by the CB1 receptor. In this work we synthesized 18 biphenylic carboxamides as new CB2-selective ligands and evaluated their pharmacological profiles. The functional activity of these compounds is strongly influenced by the nature of the substituent at position 4′ and 5 of the biphenyl scaffold. Position 5 seems to be responsible for the agonist or inverse agonist behaviour independently of the substituent in position 4′, with the exception of the methoxyl group which transforms both full agonists and inverse agonists into neutral antagonists. This study provides a novel complete toolbox of CB2 functional modulators that derive from the same chemical scaffold. Such probes may be useful to investigate the biological role of CB2 receptors in cellular assays.
Copyright © 2016 Elsevier Masson SAS. All rights reserved.
Copyright © 2016 Elsevier Masson SAS. All rights reserved.
KEYWORDS:
Biphenyl-carboxamides; CB(2); CB(2) agonist; CB(2) antagonist; CB(2) inverse agonist; Cannabinoid receptor; Endocannabinoid system; Methylhonokiol
- PMID:
- 27078864
- [PubMed – as supplied by publisher]