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作者 |
Bettini, E; Sava, A; Griffante, C; Carignani, C; Buson, A; Capelli, AM; Negri, M; Andreetta, F; Senar-Sancho, SA; Guiral, L; Cardullo, F |
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[摘要]:NR1/NR2A is a subtype of N-methyl-D-aspartate receptors (NMDARs), which are glutamate and glycine-gated Ca2+ permeable channels highly expressed in the central nervous system. A high-throughput screening (HTS) campaign using human osteosarcoma (U-2 OS) cells transiently transduced with NR1/NR2A NMDAR subunits, tested in a specifically designed fluorometric imaging plate reader (FLIPR)/Ca2+ assay, identified sulfonamide derivative series, exemplified by 3-chloro-4-fluoro-N-[(4-{[2-(phenylcarbonyl) hydrazino] carbonyl} phenyl) methyl] benzenesulfonamide (compound 1) and thiodiazole derivative N-(cyclohexylmethyl)-2-({5[(phenylmethyl) amino]-1,3,4-thiadiazol-2-yl} thio) acetamide (compound 13) as novel NR1/NR2A receptor antagonists. Compounds 1 and 13 displayed submicromolar and micromolar potency at NR1/NR2A receptor, respectively, although they did not show activity at NR2B-containing receptor up to 50 mu M concentration. Addition of 1 mM glycine, but not 1 mM L-glutamate, was able to surmount compound 1 and 13 inhibitory effects in FLIPR NR1/NR2A assay. However, compounds 1 and 13 displaced a glutamate site antagonist [H-3]D,L-(E)-2-amino-4-propyl-5-phosphono-3-pentenoic acid ([H-3]CGP 39653) to a greater extent than the glycine site antagonist [H-3]3-[(E)-2-carboxy-2-phenylethenyl]-4,6dichloro-1H-indole-2-carboxylic acid ([H-3]MDL 105,519), in rat brain cortex binding assay. Results of FLIPR cell-based, electrophysiological, and biochemical binding assays suggest that compounds 1 and 13 are the prototypes of novel classes of NMDAR ligands, which to the best of our knowledge are the first selective antagonists at NR1/NR2A over NR1/NR2B receptor, and might constitute useful tools able to elucidate the relative role of the NR2A subunit in physiological and pathological conditions. |
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