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Development of squaramides as allosteric modulators of the cb1 receptor
Synthesis, computational studies, biological characterization, and effects against cocaine-induced behavioral sensitization and reinstatement in rats
Nguyen, T., Decker, A. M., Barrus, D. G., Song, C. H., Liu, J., Gamage, T. F., Harris, D. L., Li, J.-X., & Zhang, Y. (2025). Development of squaramides as allosteric modulators of the cb1 receptor: Synthesis, computational studies, biological characterization, and effects against cocaine-induced behavioral sensitization and reinstatement in rats. Journal of Medicinal Chemistry, 68(8), 8694-8712. https://doi.org/10.1021/acs.jmedchem.5c00383
Cannabinoid receptor type 1 (CB1) negative allosteric modulators have emerged as an alternate approach to CB1 orthosteric antagonists/inverse agonists for cocaine addiction treatment. This study explores aryl-alkyl squaramides as CB1 allosteric modulators, featuring RTICBM-262 (3) with good in vitro potencies in CB1 calcium mobilization, [35S]GTP gamma S binding, and cAMP assays. Molecular modeling studies suggest 3 bound in a similar pocket as Org27569, forming pi-stacking with key residues H1542.41 and W2414.50, and the potential C98-C107 disulfide bond had limited impact on its binding or receptor activation. ADME and in vivo pharmacokinetic studies suggest that 3 had reasonable metabolic stability, brain penetration, and selectivity against a panel of similar to 50 targets but poor solubility and high protein binding. At 5.6 mg/kg (i.p.), 3 significantly attenuated both cocaine-seeking behavior specific to cue-induced reinstatement and cocaine-induced behavioral sensitization without altering locomotor activity. These results support squaramides as promising candidates for further investigation for cocaine addiction treatment.
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