Synthesis and biological evaluation of novel N-substituted nipecotic acid derivatives with tricyclic cage structures in the lipophilic domain as GABA uptake inhibitors

被引:0
|
作者
Heinrich-Karl A. Rudy
Georg Höfner
Klaus T. Wanner
机构
[1] Department of Pharmacy – Center for Drug Research,
[2] Ludwig-Maximilians-Universität München,undefined
来源
Medicinal Chemistry Research | 2021年 / 30卷
关键词
GABA transporters; GABA uptake inhibitor; Nipecotic acid; Polycycles; Cage structures;
D O I
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中图分类号
学科分类号
摘要
A new class of GABA reuptake inhibitors with sterically demanding, highly rigid tricyclic cage structures as the lipophilic domain was synthesized and investigated in regard to their biological activity at the murine GABA transporters (mGAT1–mGAT4). The construction of these compounds, consisting of nipecotic acid, a symmetric tricyclic amine, and a plain hydrocarbon linker connecting the two subunits via their amino nitrogens, was accomplished via reductive amination of a nipecotic acid derivative with an N-alkyl substituent displaying a terminal aldehyde function with tricyclic secondary amines. The target compounds varied with regard to spacer length, the bridge size of one of the bridges, and the substituents of the tricyclic skeleton to study the impact of these changes on their potency. Among the tested compounds nipecotic acid ethyl ester derivates with phenyl residues attached to the cage subunit showed reasonable inhibitory potency and subtype selectivity in favor of mGAT3 and mGAT4, respectively.
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页码:586 / 609
页数:23
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