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使用生物物理和计算技术对3-芳酰基-2-甲基咪唑并[1,2 -]嘧啶与牛血清白蛋白进行多组分无催化剂区域选择性合成及结合研究。

Multicomponent catalyst-free regioselective synthesis and binding studies of 3-aroyl-2-methylimidazo[1,2-]pyrimidines with BSA using biophysical and computational techniques.

作者信息

Aggarwal Ranjana, Sharma Manisha, Sumran Garima, Kumar Parvin

机构信息

Department of Chemistry, Kurukshetra University Kurukshetra-136119 Haryana India.

Council of Scientific and Industrial Research-National Institute of Science Communication and Policy Research New Delhi 110012 India

出版信息

RSC Adv. 2025 May 14;15(20):15999-16014. doi: 10.1039/d5ra01795e. eCollection 2025 May 12.

DOI:10.1039/d5ra01795e
PMID:40370858
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12076138/
Abstract

A facile and environmentally benign protocol for regioselective synthesis of diversely substituted imidazo[1,2-]pyrimidines 5a-h has been described multicomponent reaction of unsymmetrical β-diketones 1, -bromosuccinimide 2 and 2-aminopyrimidine 4 in DCM. The reaction proceeds through formation of α-bromo-β-diketones 3 and their ensuing condensation with 2-aminopyrimidine without the need of any organic or inorganic catalyst. The structure of the regioisomeric product was characterized by H, C NMR, heteronuclear 2D NMR and HRMS studies. The present protocol offers several advantages such as avoidance of metal-based and toxic catalysts, broad substrate scope with respect to substitutions on β-diketones, operational simplicity, easy work-up and high yields. Computational molecular docking studies were carried out to examine the interaction of imidazo[1,2-]pyrimidines with bovine serum albumin (BSA). Moreover, different spectroscopic approaches UV-visible, steady-state fluorescence and competitive displacement assays were carried out to investigate the binding mechanisms of imidazo[1,2-]pyrimidines (5c, 5e and 5h) with BSA. The results thus obtained revealed that imidazo[1,2-]pyrimidines showed moderate binding with BSA through a static quenching mechanism and compound 5e had more affinity to bind in site I of BSA.

摘要

已描述了一种简便且环境友好的区域选择性合成多种取代的咪唑并[1,2 - ]嘧啶5a - h的方法,该方法是在二氯甲烷中使不对称β - 二酮1、N - 溴代琥珀酰亚胺2和2 - 氨基嘧啶4进行多组分反应。该反应通过形成α - 溴代β - 二酮3并随后与2 - 氨基嘧啶缩合进行,无需任何有机或无机催化剂。通过氢谱、碳谱、异核二维核磁共振和高分辨质谱研究对区域异构体产物的结构进行了表征。本方法具有多种优点,如避免使用金属基和有毒催化剂、β - 二酮取代基的底物范围广、操作简单、后处理容易且产率高。进行了计算分子对接研究以考察咪唑并[1,2 - ]嘧啶与牛血清白蛋白(BSA)的相互作用。此外,还采用了不同的光谱方法——紫外可见光谱、稳态荧光光谱和竞争置换测定法来研究咪唑并[1,2 - ]嘧啶(5c、5e和5h)与BSA的结合机制。由此获得的结果表明,咪唑并[1,2 - ]嘧啶通过静态猝灭机制与BSA表现出适度结合,且化合物5e在BSA的位点I具有更强的结合亲和力。

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