DESIGN, SYNTHESIS AND PHARMACOLOGICAL EVALUATION OF NOVEL N- {4-[2-(4-ARYL-PIPERAZIN-1-YL)-ETHYL]-PHENYL}-ARYLAMIDES

D. Andrić, Slađana Dukić-Stefanovic, J. Penjišević, I. Jevtić, V. Šukalović, Relja Suručić, Slađana V. Kostić-Rajačić
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Abstract

5HT1A receptor targeting drugs have been used as the treatment for the many neuropsychiatric disorders, such as schizophrenia and depression. As a part of ongoing research, we designed series of new compounds that share arylpiperazine common structural motif with the 5HT1A receptor ligand aripiprazole. Receptor-ligand interactions were determined by the molecular docking simulations, revealing the positive impact of the phenyl substitution in the arylpiperazine part of the molecules. Nine selected compounds were synthesized in four reaction steps in high overall yields (59-73%). In vitro pharmacological evaluation of the synthesized compounds revealed three compounds (5b, 6b and 6c) with high 5HT1A binding affinity, comparable with aripiprazole (Ki 12.0, 4.8, 12.8, 5.6 nM, respectively). Compounds from b series, 5b and 6b, possess 2-methoxyphenyl substituents, while 6c possess 2,3-dichlorophenyl substituent in the arylpiperazine part of the molecule. The pharmacological results are therefore in accordance with the molecular docking simulations thus proving the rational design. Compounds 5c, 6b and 6c can be considered as the candidates for further evaluation as new, potential antidepressants.
新型n -{4-[2-(4-芳基-哌嗪-1-基)-乙基]-苯基}芳基酰胺的设计、合成及药理评价
5HT1A受体靶向药物已被用于治疗许多神经精神疾病,如精神分裂症和抑郁症。作为正在进行的研究的一部分,我们设计了一系列与5HT1A受体配体阿立哌唑具有芳基哌嗪共同结构基序的新化合物。通过分子对接模拟确定了受体与配体的相互作用,揭示了分子中芳基哌嗪部分的苯基取代的积极影响。选定的9个化合物经过4个反应步骤合成,总收率较高(59 ~ 73%)。体外药理学评价显示,3个化合物(5b、6b和6c)具有与阿立哌唑相当的高5HT1A结合亲和力(Ki分别为12.0、4.8、12.8和5.6 nM)。b系化合物5b和6b在芳基哌嗪部分具有2-甲氧基取代基,6c在芳基哌嗪部分具有2,3-二氯苯取代基。因此,药理学结果与分子对接模拟一致,从而证明了设计的合理性。化合物5c、6b和6c可作为新的、潜在的抗抑郁药进行进一步评价。
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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