Cannabielsoin (CBE), a CBD Oxidation Product, Is a Biased CB1 Agonist

Author:

Haghdoost Mehdi1,Young Scott2,Roberts Matthew1,Krebs Caitlyn1,Bonn-Miller Marcel O.2

Affiliation:

1. Nalu Bio Inc., 38 Keyes Avenue, Suite 117, San Francisco, CA 94129, USA

2. Charlotte’s Web, 700 Tech Court, Louisville, CO 80027, USA

Abstract

Cannabielsoin (CBE) is primarily recognized as an oxidation byproduct of cannabidiol (CBD) and a minor mammalian metabolite of CBD. The pharmacological interactions between CBE and cannabinoid receptors remain largely unexplored, particularly with respect to cannabinoid receptor type 1 (CB1). The present study aimed to elucidate the interaction dynamics of CBE in relation to CB1 by employing cyclic adenosine monophosphate (cAMP) and β-arrestin assays to assess its role as an agonist, antagonist, and positive allosteric modulator (PAM). To our knowledge, this is the first publication to investigate CBE’s receptor activity in vitro. Our findings reveal that S-CBE acts as an agonist to CB1 with EC50 = 1.23 µg/mL (3.7 µM) in the cAMP assay. No agonist activity was observed in the β-arrestin assay in concentrations up to 12 µM, suggesting a noteworthy affinity towards G-protein activation and the cAMP signaling pathway. Furthermore, in silico molecular docking simulations were conducted to provide a structural basis for the interaction between CBE and CB1, offering insights into the molecular determinants of its receptor affinity and functional selectivity.

Funder

Charlotte’s Web

Publisher

MDPI AG

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