针对5-HT1A和Sigma-1受体的新型芳基哌嗪的设计、合成及抗抑郁活性研究

Pharmaceutical Fronts Pub Date : 2021-12-25 DOI:10.1055/s-0041-1740049

Yan-Na Ni, Xin-Li Du, Tao Wang, Yuanbin Chen, Xiang-qing Xu, Song Zhao, Jian-qi Li, Guan Wang

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引用次数: 0

摘要

设计合成了20个新的芳基哌嗪衍生物，并通过质谱分析和核磁共振分析对其结构进行了确证。测定了它们的5-HT1A和sigma-1受体亲和性，其中6个对5-HT1A和sigma-1靶点均表现出高亲和性(ki < 20 nmol/L)。然后进行了6种化合物在大鼠和人肝微粒体中的代谢稳定性(t1 /2)试验。我们的数据表明，化合物27对5-HT1A和sigma-1受体都有很高的亲和力(5-HT1A: K i = 0.44 nmol/L;σ -1: K i = 0.27 nmol/L)，代谢稳定性好(t1 /2值分别为21.7和24.6分钟)。有趣的是，强迫游泳试验、小鼠悬尾试验和初步药代动力学试验结果表明，化合物27在两种模型中均具有明显的抗抑郁活性、良好的药代动力学特性和低毒性。综上所述，化合物27作为抗抑郁药物的活性分子具有进一步研究的价值。

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Design, Synthesis, and Antidepressant Activity Study of Novel Aryl Piperazines Targeting Both 5-HT1A and Sigma-1 Receptors

A total of 20 novel aryl piperazine derivatives were designed and synthesized, and their structures were confirmed by mass spectrometry and nuclear magnetic resonance analyses. Their 5-HT1A and sigma-1 receptor affinities were determined, and six of them showed high affinities (K i < 20 nmol/L) to both 5-HT1A and sigma-1 targets. Then, metabolic stability (T 1/2) tests of six compounds in rat and human liver microsomes were performed. Our data indicated that compound 27 has both high affinity for 5-HT1A and sigma-1 receptors (5-HT1A: K i = 0.44 nmol/L; sigma-1: K i = 0.27 nmol/L), and good metabolic stability (T 1/2 values are 21.7 and 24.6 minutes, respectively). Interestingly, results from the forced swimming test, mouse tail suspension test, and preliminary pharmacokinetic test suggested the marked antidepressant activity, good pharmacokinetic characteristics, and low toxicity of compound 27 in the two models. In conclusion, compound 27 has great value of further study as an active molecule of antidepressant drugs.

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Pharmaceutical Fronts

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审稿时长

15 weeks