| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1395525 | European Journal of Medicinal Chemistry | 2015 | 12 Pages |
•New analogues of agomelatine were synthesized and tested.•Combination of β- and C-3 modulations led to compounds with good pharmacological profile.•Synthesized series conserved good melatonin binding affinities.•The allyl 7b and ethyl 16a represented the most interesting compounds of this series.
In this paper we report the investigation of C-3 and β-acetamide positions of agomelatine analogues. Concomitant insertion of a hydroxymethyl in the β-acetamide position and aliphatic groups in C-3 position produced a positive effect on both melatonin (MT1, MT2) and serotonin (5-HT2C) binding affinities. In particular, the allyl 6b and ethyl 15a represented the more interesting compounds of this series. Furthermore, the introduction of methyl cycloalkyl groups (compounds 11a, 12a) exhibited no change in both MT2 and 5-HT2C binding affinities while a decrease of MT1 binding affinity occurred leading to an MT2 selectivity. Finally, the acetamide modulation has led to methyl thiourea 11h, with a weak MT2 selectivity.
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