Mastering tricyclic ring systems for desirable functional cannabinoid activity

Petrov, Ravil R.; Knight, Lindsay K.; Chen, Shao Rui; Wager-Miller, Jim; McDaniel, Steven W.; Diaz, Fanny; Barth, Francis; Pan, Hui Lin; Mackie, Ken; Cavasotto, Claudio N.; Diaz, Philippe

doi:10.1016/j.ejmech.2013.09.038

Cited by 40 publications

(31 citation statements)

References 60 publications

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“…The structure of MDMB-CHMCZCA, a semi-systematic name for m ethyl d i m ethyl b utanoate- c yclo h exyl m ethyl c arba z ole c arbox a mide, is related to the structure of MDMB-CHMICA, but contains an N -alkylated carbazole instead of an indole core. Carbazoles are the core structures of an emerging group of cannabimimetics [11–12]. Several N -alkylated carbazole-3-carboxamides were patented by Diaz, Diaz, and Petrov in 2012 as tricyclic cannabinoid receptor modulators, explored against neuropathic pain [13].…”

Section: Introductionmentioning

confidence: 99%

Characterization of the synthetic cannabinoid MDMB-CHMCZCA

Weber¹,

Pusch²,

Schollmeyer³

et al. 2016

Beilstein J. Org. Chem.

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The synthetic cannabinoid MDMB-CHMCZCA was characterized by various spectroscopic techniques including NMR spectroscopy and tandem mass spectrometry. The synthetic sample was found to be of S-configuration by VCD spectroscopy and comparison of the data with DFT calculations, while ECD spectroscopy was found to be inconclusive in this case. The enantiomeric purity of samples from test purchases and police seizures was assessed by a self-developed chiral HPLC method.

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Section: Introductionmentioning

confidence: 99%

Characterization of the synthetic cannabinoid MDMB-CHMCZCA

Weber¹,

Pusch²,

Schollmeyer³

et al. 2016

Beilstein J. Org. Chem.

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“…Thus, internalization of a GPCR in response to a ligand can be considered a form of signaling. CB 2 receptors exhibit variable internalization in response to an agonist, with some agonists promoting marked internalization and others being inactive (Grimsey et al, 2011;Atwood et al, 2012b;Petrov et al, 2013).…”

Section: Ion Channelsmentioning

confidence: 99%

CB₂Cannabinoid Receptors as a Therapeutic Target—What Does the Future Hold?

2014

Self Cite

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The past decades have seen an exponential rise in our understanding of the endocannabinoid system, comprising CB 1 and CB 2 cannabinoid receptors, endogenous cannabinoids (endocannabinoids), and the enzymes that synthesize and degrade endocannabinoids. The primary focus of this review is the CB 2 receptor. CB 2 receptors have been the subject of considerable attention, primarily due to their promising therapeutic potential for treating various pathologies while avoiding the adverse psychotropic effects that can accompany CB 1 receptor-based therapies. With the appreciation that CB 2 -selective ligands show marked functional selectivity, there is a renewed opportunity to explore this promising area of research from both a mechanistic as well as a therapeutic perspective. In this review, we summarize our present knowledge of CB 2 receptor signaling, localization, and regulation. We discuss the availability of genetic tools (and their limitations) to study CB 2 receptors and also provide an update on preclinical data on CB 2 agonists in pain models. Finally, we suggest possible reasons for the failure of CB 2 ligands in clinical pain trials and offer possible ways to move the field forward in a way that can help reconcile the inconsistencies between preclinical and clinical data.

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“…In cases of low sequence similarity, multiple sequence alignment might help in improving the quality of the final model [45][46][47], though it should be stressed that a correct sequence alignment is necessary -though hardly sufficient-to develop reliable homology models. Regarding the construction of the crude model, multiple-template approaches have also been used to model the target "by pieces" [48][49][50][51][52].…”

Section: In Silico Target Models In Structure-based Virtual Screeningmentioning

confidence: 99%

“…Later, a benchmarking study for existing GPCRs was published [41] (see next section). The ligand steered method was also used to rationalize structure-activity relationships (SAR) data of agonists and antagonists binding to the cannabinoid CB2 receptor [49,51,68].…”

Section: Integral Binding-site Modeling and Refinementmentioning

confidence: 99%