Design,synthesis and activity evaluation of novel 5-HT2A receptor antagonists
10.7644/j.issn.1674-9960.2024.10.007
- VernacularTitle:新型5-羟色胺2A受体拮抗剂的设计、合成及活性评价
- Author:
Luobing HAN
1
;
Shiyang SUN
;
Yu ZHAO
;
Gang YU
;
Ruibin SU
;
Zhibing ZHENG
;
Song LI
Author Information
1. 军事科学院军事医学研究院国家安全特需药品全国重点实验室,北京 100850
- Keywords:
5-HT2A receptor;
antagonists;
drug design;
Parkinson's disease psychosis;
chemical synthesis;
anti-hallu-cinations
- From:
Military Medical Sciences
2024;48(10):767-777
- CountryChina
- Language:Chinese
-
Abstract:
Objective To discover 5-HT2A receptor antagonist molecules with novel structures and explore their structure-activity relationship through structure-and mechanism-based drug design,synthesis and activity evaluation.Methods The way in which pimovanserin interacted with 5-HT2A receptor was analyzed via molecular docking,molecular dynamics simulation and binding free energy calculations.Based on the results of this study,the 5-HT2A receptor antagonist target compounds with novel structures were designed using pimovanserin as the lead molecule.According to the structures of target compounds,corresponding synthetic routes were designed.The heterocyclic methylamine intermediates were obtained by reductive amination or reduction reaction from heterocyclic formaldehyde or heterocyclic methanonitrile before being reacted with 4-(4-fluorobenzylamino)-1-methylpiperidine to obtain the target compounds using CDI urea synthesis method.The inhibitory activity of the target compounds against 5-HT2A receptor was tested at the cellular level,and the anti-hallucinogenic effects of the target compounds were tested in the mouse head twitch response model.Results Twelvenovel compounds were synthesized and their structures were confirmed by HR-MS,1H-NMR and 13C-NMR.The results of the activity assay showed that compounds 6a,6c and 6d exhibited better 5-HT2Areceptor inhibitoryactivity with IC50 values of 120,152 and 285 nmol/L,respectively while compounds 6c and 6d exhibited better anti-hallucinogenic activity in mice with inhibition rates of 97.0%and 82.9%(10 mg/kg),respectively.Conclusion The novel compound 6c and 6d have shown strong 5-HT2A receptor inhibitoryactivity and anti-hallucinogenic activity and deserve more research.Structure-activity relationship analyses of target compounds indicate that the repulsion of the heterocyclic ring with basic N atoms and the accommodation of the heterocyclic ring without basic N atoms by the side extended pocket of the 5-HT2A receptor could significantly affect the ex vivo and in vivo effects of antagonists.
