Investigations on the 4-Quinolone-3-Carboxylic Acid Motif Part 5: Modulation of the Physicochemical Profile of a Set of Potent and Selective Cannabinoid-2 Receptor Ligands through a Bioisosteric Approach

Claudia Mugnaini; Stefania Nocerino; Valentina Pedani; Serena Pasquini; Andrea Tafi; Maria De Chiaro; Luca Bellucci; Massimo Valoti; Francesca Guida; Livio Luongo; Stefania Dragoni; Alessia Ligresti; Avraham Rosenberg; Daniele Bolognini; Maria Grazia Cascio; Roger G Pertwee; Ruin Moaddel; Sabatino Maione; Vincenzo Di Marzo; Federico Corelli

doi:10.1002/cmdc.201100573

Investigations on the 4-Quinolone-3-Carboxylic Acid Motif Part 5: Modulation of the Physicochemical Profile of a Set of Potent and Selective Cannabinoid-2 Receptor Ligands through a Bioisosteric Approach

Claudia Mugnaini, Stefania Nocerino, Valentina Pedani, Serena Pasquini, Andrea Tafi, Maria De Chiaro, Luca Bellucci, Massimo Valoti, Francesca Guida, Livio Luongo, Stefania Dragoni, Alessia Ligresti, Avraham Rosenberg, Daniele Bolognini, Maria Grazia Cascio, Roger G Pertwee, Ruin Moaddel, Sabatino Maione, Vincenzo Di Marzo, Federico Corelli

Medical Sciences

Research output: Contribution to journal › Article › peer-review

31 Citations (Scopus)

Abstract

Three heterocyclic systems were selected as potential bioisosteres of the amide linker for a series of 1,6-disubstituted-4-quinolone-3-carboxamides, which are potent and selective CB2 ligands that exhibit poor water solubility, with the aim of improving their physicochemical profile and also of clarifying properties of importance for amide bond mimicry. Among the newly synthesized compounds, a 1,2,3-triazole derivative (1-(adamantan-1-yl)-4-[6-(furan-2-yl)-1,4-dihydro-4-oxo-1-pentylquinolin-3-yl]-1H-1,2,3-triazole) emerged as the most promising in terms of both physicochemical and pharmacodynamic properties. When assayed in vitro, this derivative exhibited inverse agonist activity, whereas, in the formalin test in mice, it produced analgesic effects antagonized by a well-established inverse agonist. Metabolic studies allowed the identification of a side chain hydroxylated derivative as its only metabolite, which, in its racemic form, still showed appreciable CB2 selectivity, but was 150-fold less potent than the parent compound.

Original language	English
Pages (from-to)	920-934
Number of pages	15
Journal	ChemMedChem
Volume	7
Issue number	5
Early online date	2 Mar 2012
DOIs	https://doi.org/10.1002/cmdc.201100573
Publication status	Published - May 2012

Keywords

bioisosteres
cannabinoids
quinolones
receptors
structure-activity relationship

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10.1002/cmdc.201100573

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Mugnaini, C., Nocerino, S., Pedani, V., Pasquini, S., Tafi, A., De Chiaro, M., Bellucci, L., Valoti, M., Guida, F., Luongo, L., Dragoni, S., Ligresti, A., Rosenberg, A., Bolognini, D., Cascio, M. G., Pertwee, R. G., Moaddel, R., Maione, S., Di Marzo, V., & Corelli, F. (2012). Investigations on the 4-Quinolone-3-Carboxylic Acid Motif Part 5: Modulation of the Physicochemical Profile of a Set of Potent and Selective Cannabinoid-2 Receptor Ligands through a Bioisosteric Approach. ChemMedChem, 7(5), 920-934. https://doi.org/10.1002/cmdc.201100573

Investigations on the 4-Quinolone-3-Carboxylic Acid Motif Part 5: Modulation of the Physicochemical Profile of a Set of Potent and Selective Cannabinoid-2 Receptor Ligands through a Bioisosteric Approach. / Mugnaini, Claudia; Nocerino, Stefania; Pedani, Valentina et al.
In: ChemMedChem, Vol. 7, No. 5, 05.2012, p. 920-934.

Research output: Contribution to journal › Article › peer-review

Mugnaini, C, Nocerino, S, Pedani, V, Pasquini, S, Tafi, A, De Chiaro, M, Bellucci, L, Valoti, M, Guida, F, Luongo, L, Dragoni, S, Ligresti, A, Rosenberg, A, Bolognini, D, Cascio, MG , Pertwee, RG, Moaddel, R, Maione, S, Di Marzo, V & Corelli, F 2012, 'Investigations on the 4-Quinolone-3-Carboxylic Acid Motif Part 5: Modulation of the Physicochemical Profile of a Set of Potent and Selective Cannabinoid-2 Receptor Ligands through a Bioisosteric Approach', ChemMedChem, vol. 7, no. 5, pp. 920-934. https://doi.org/10.1002/cmdc.201100573

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abstract = "Three heterocyclic systems were selected as potential bioisosteres of the amide linker for a series of 1,6-disubstituted-4-quinolone-3-carboxamides, which are potent and selective CB2 ligands that exhibit poor water solubility, with the aim of improving their physicochemical profile and also of clarifying properties of importance for amide bond mimicry. Among the newly synthesized compounds, a 1,2,3-triazole derivative (1-(adamantan-1-yl)-4-[6-(furan-2-yl)-1,4-dihydro-4-oxo-1-pentylquinolin-3-yl]-1H-1,2,3-triazole) emerged as the most promising in terms of both physicochemical and pharmacodynamic properties. When assayed in vitro, this derivative exhibited inverse agonist activity, whereas, in the formalin test in mice, it produced analgesic effects antagonized by a well-established inverse agonist. Metabolic studies allowed the identification of a side chain hydroxylated derivative as its only metabolite, which, in its racemic form, still showed appreciable CB2 selectivity, but was 150-fold less potent than the parent compound.",

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author = "Claudia Mugnaini and Stefania Nocerino and Valentina Pedani and Serena Pasquini and Andrea Tafi and {De Chiaro}, Maria and Luca Bellucci and Massimo Valoti and Francesca Guida and Livio Luongo and Stefania Dragoni and Alessia Ligresti and Avraham Rosenberg and Daniele Bolognini and Cascio, {Maria Grazia} and Pertwee, {Roger G} and Ruin Moaddel and Sabatino Maione and {Di Marzo}, Vincenzo and Federico Corelli",

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AU - Nocerino, Stefania

AU - Pedani, Valentina

AU - Pasquini, Serena

AU - Tafi, Andrea

AU - De Chiaro, Maria

AU - Bellucci, Luca

AU - Valoti, Massimo

AU - Guida, Francesca

AU - Luongo, Livio

AU - Dragoni, Stefania

AU - Ligresti, Alessia

AU - Rosenberg, Avraham

AU - Bolognini, Daniele

AU - Cascio, Maria Grazia

AU - Pertwee, Roger G

AU - Moaddel, Ruin

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AU - Di Marzo, Vincenzo

AU - Corelli, Federico

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Investigations on the 4-Quinolone-3-Carboxylic Acid Motif Part 5: Modulation of the Physicochemical Profile of a Set of Potent and Selective Cannabinoid-2 Receptor Ligands through a Bioisosteric Approach

Abstract

Keywords

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