Synthesis and 5-HT3 receptor affinity of new quinolinecarboxylic acid derivatives.

Drug design and discovery Pub Date : 2000-01-01
A Orjales, L Alonso-Cires, P L López-Tudanca, I Tapia, L Labeaga, R Mosquera
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Abstract

A series of quinolinecarboxylic acid amides and an ester with a quinuclidine moiety were synthesized and their in vitro affinities at 5-HT3, 5-HT4, and D2 receptors evaluated by radioligand binding assays. Highest affinity at 5-HT3 receptor corresponded to derivative 5 with Ki = 9.9 nM and with selectivity over 5-HT4 and D2 receptors. Compounds displayed moderate 5-HT3 antagonist activity (ED50 = 10.5-21.5 microg/kg i.v.). The obtained data suggest that the 5-HT3 receptor sites can accommodate the acyl group of the 2-quinoline derivatives. The results indicate the existence of an optimal distance between the lone electron pair of the quinoline nitrogen atom and the azabicyclic nitrogen atom, and a no-pharmacophoric pocket in the 5-HT3 receptor which would hold the fragment at the position 4 of the quinoline ring.

新型喹啉羧酸衍生物的合成及其5-HT3受体亲和力。
合成了一系列喹啉羧酸酰胺和一种含有喹啉基片段的酯,并通过放射配体结合试验评估了它们与5-HT3、5-HT4和D2受体的体外亲和力。与5- ht3受体亲和度最高的衍生物5 Ki = 9.9 nM,对5- ht4和D2受体具有选择性。化合物表现出中等的5-HT3拮抗剂活性(ED50 = 10.5-21.5 μ g/kg静脉注射)。得到的数据表明,5-HT3受体位点可以容纳2-喹啉衍生物的酰基。结果表明,喹啉氮原子的孤电子对与氮杂环氮原子之间存在一个最佳距离,并且5-HT3受体中存在一个无药效口袋,该口袋可将片段保存在喹啉环的第4位。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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