四唑和恶二唑衍生物作为塔里奎达和依拉奎达的生物同位体:作为MDR逆转剂的新型强效P-gp调节剂。

IF 6 2区 医学 Q1 CHEMISTRY, MEDICINAL European Journal of Medicinal Chemistry Pub Date : 2023-11-05 DOI:10.1016/j.ejmech.2023.115716
Laura Braconi , Silvia Dei , Marialessandra Contino , Chiara Riganti , Gianluca Bartolucci , Dina Manetti , Maria Novella Romanelli , Maria Grazia Perrone , Nicola Antonio Colabufo , Stefano Guglielmo , Elisabetta Teodori
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引用次数: 1

摘要

合成了新的2,5-和1,5-二取代四唑,以及2,5-二取代-1,3,4-恶二唑作为塔里奎达和埃拉奎达衍生物,并作为多药耐药性(MDR)逆转剂进行了研究。研究了它们对三种ABC转运蛋白P-gp、MRP1和BCRP的作用。所有化合物都抑制过表达P-gp的MDCK-MDR1细胞中的P-gp转运活性,即使在低纳摩尔范围内也显示出EC50值(化合物15,22)。恶二唑衍生物能够增加阿霉素在MDCK-MDR1和HT29/DX细胞中的抗增殖作用,证实了其P-gp调节剂的性质,其中衍生物15在这些测定中是最有效的。化合物15还显示出对P-gp和BCRP都显示出良好活性的双重抑制作用。一项计算研究表明,大多数强效化合物在P-gp上有一种常见的相互作用模式。先导化合物酰胺基的生物同位取代允许鉴定一组新的强效恶二唑衍生物,其通过抑制P-gp外排活性来调节MDR。如果与以前的酰胺衍生物相比,杂环环的引入极大地增强了对P-gp的活性,在两种化合物中引入了对MRP1的中等抑制活性,并且在某些情况下保持了对BCRP的作用,从而揭示了双重抑制剂15。
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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Tetrazole and oxadiazole derivatives as bioisosteres of tariquidar and elacridar: New potent P-gp modulators acting as MDR reversers

New 2,5- and 1,5-disubstituted tetrazoles, and 2,5-disubstituted-1,3,4-oxadiazoles were synthesized as tariquidar and elacridar derivatives and studied as multidrug resistance (MDR) reversers. Their behaviour on the three ABC transporters P-gp, MRP1 and BCRP was investigated. All compounds inhibited the P-gp transport activity in MDCK-MDR1 cells overexpressing P-gp, showing EC50 values even in the low nanomolar range (compounds 15, 22). Oxadiazole derivatives were able to increase the antiproliferative effect of doxorubicin in MDCK-MDR1 and in HT29/DX cells confirming their nature of P-gp modulators, with derivative 15 being the most potent in these assays. Compound 15 also displayed a dual inhibitory effect showing good activities towards both P-gp and BCRP. A computational study suggested a common interaction pattern on P-gp for most of the potent compounds. The bioisosteric substitution of the amide group of lead compounds allowed identifying a new set of potent oxadiazole derivatives that modulate MDR through inhibition of the P-gp efflux activity. If compared to previous amide derivatives, the introduction of the heterocycle rings greatly enhances the activity on P-gp, introduces in two compounds a moderate inhibitory activity on MRP1 and maintains in some cases the effect on BCRP, leading to the unveiling of dual inhibitor 15.

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来源期刊
CiteScore
11.70
自引率
9.00%
发文量
863
审稿时长
29 days
期刊介绍: The European Journal of Medicinal Chemistry is a global journal that publishes studies on all aspects of medicinal chemistry. It provides a medium for publication of original papers and also welcomes critical review papers. A typical paper would report on the organic synthesis, characterization and pharmacological evaluation of compounds. Other topics of interest are drug design, QSAR, molecular modeling, drug-receptor interactions, molecular aspects of drug metabolism, prodrug synthesis and drug targeting. The journal expects manuscripts to present the rational for a study, provide insight into the design of compounds or understanding of mechanism, or clarify the targets.
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