芬太尼三唑衍生物的合成及其对mu -阿片和Sigma-1受体的亲和力

IF 1.3 4区 化学 Q3 CHEMISTRY, MULTIDISCIPLINARY
Ruth Paulino, R. Alves, Joanna Matalińska, Piotr F. J. Lipiński, R. Freitas
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引用次数: 0

摘要

寻找同时与mu-阿片受体(MOR)和sigma-1受体(σ1R)具有亲和力的化合物是开发低副作用止痛药的创新方向之一。此外,在过去的二十年中,三唑支架在药物化学中得到了广泛的探索。在此背景下,我们合成了一系列新的三唑芬太尼衍生物,并评估了它们对MOR和σ1R的亲和力。以芬太尼为标准,采用竞争性放射配体结合法测定化合物对人MOR的结合亲和力。采用σ1R激动剂SKF10047进行测定。活性最高的类似物为6d,与MOR的半抑制浓度(IC50)为1.9 μM,与σ1R的半抑制浓度(IC50)为6.9 μM。进行了分子对接计算,对观察到的亲和值进行了结构解析。使用SwissADME工具模拟新化合物的吸收、分布、代谢和排泄毒性(ADMET)参数
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Synthesis of Fentanyl Triazole Derivatives and their Affinity for Mu-Opioid and Sigma-1 Receptors
The search for compounds with affinity for both mu-opioid receptor (MOR) and sigma-1 receptor (σ1R) is one of the innovative directions to develop painkillers with reduced side effects. Additionally, triazole scaffolds have been extensively explored in the last two decades in medicinal chemistry. In this context, we synthesized a series of new triazole fentanyl derivatives and evaluated their affinity for both MOR and σ1R. The binding affinity of the compounds for human MOR was determined in competitive radioligand binding assays, using fentanyl as standard. For the assays with σ1R, a σ1R agonist (SKF10047) was employed. The most active analogue was 6d which moderately binds to MOR with half-maximal inhibitory concentrations (IC50) = 1.9 μM and to σ1R with IC50 = 6.9 μM. Molecular docking calculations were carried out, providing a structural elucidation for the observed values of affinity. Absorption, distribution, metabolism, and excretion toxicity (ADMET) parameters for the new compounds were simulated with the SwissADME tool
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来源期刊
CiteScore
2.90
自引率
7.10%
发文量
99
审稿时长
3.4 months
期刊介绍: The Journal of the Brazilian Chemical Society embraces all aspects of chemistry except education, philosophy and history of chemistry. It is a medium for reporting selected original and significant contributions to new chemical knowledge.
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