新型共轭喹唑啉酮类羟肟酸的设计、合成与生物评价。

Novel Conjugated Quinazolinone-Based Hydroxamic Acids: Design, Synthesis and Biological Evaluation.

机构信息

School of Chemical Engineering, Hanoi University of Science and Technology, No 1, Dai Co Viet, Hai Ba Trung, Hanoi, Vietnam.

Institute of Natural Products Chemistry, Vietnam Academy of Science and Technology, 18-Hoang Quoc Viet-Cau Giay, Hanoi, Vietnam.

出版信息

Med Chem. 2021;17(7):732-749. doi: 10.2174/1573406416666200420081540.

DOI:10.2174/1573406416666200420081540

PMID:32310052

Abstract

BACKGROUND

The target-based approach to drug discovery currently attracts a great deal of interest from medicinal chemists in anticancer drug discovery and development. Histone deacetylase (HDAC) inhibitors represent an extensive class of targeted anti-cancer agents. Among the most explored structure moieties, hydroxybenzamides and hydroxypropenamides have been demonstrated to have potential HDAC inhibitory effects. Several compounds of these structural classes have been approved for clinical uses to treat different types of cancer, such as vorinostat and belinostat.

AIMS

This study aims at developing novel HDAC inhibitors bearing conjugated quinazolinone scaffolds with potential cytotoxicity against different cancer cell lines.

METHODS

A series of novel N-hydroxyheptanamides incorporating conjugated 6-hydroxy-2 methylquinazolin- 4(3H)-ones (15a-l) was designed, synthesized and evaluated for HDAC inhibitory potency as well as cytotoxicity against three human cancer cell lines, including HepG-2, MCF-7 and SKLu-1. Molecular simulations were finally performed to gain more insight into the structureactivity relationships.

RESULTS

It was found that among novel conjugated quinazolinone-based hydroxamic acids synthesized, compounds 15a, 15c and 15f were the most potent, both in terms of HDAC inhibition and cytotoxicity. Especially, compound 15f displayed up to nearly 4-fold more potent than SAHA (vorinostat) in terms of cytotoxicity against MCF-7 cell line with IC value of 1.86 μM, and HDAC inhibition with IC value of 6.36 μM. Docking experiments on HDAC2 isozyme showed that these compounds bound to HDAC2 with binding affinities ranging from -10.08 to -14.93 kcal/mol compared to SAHA (-15.84 kcal/mol). It was also found in this research that most of the target compounds seemed to be more cytotoxic toward SKLu-1than MCF-7 and HepG-2.

CONCLUSION

The resesrch results suggest that some hydroxamic acids could emerge for further evaluation and the results are well served as basics for further design of more potent HDAC inhibitors and antitumor agents.

摘要

背景

目前，基于靶点的药物发现方法引起了抗癌药物发现和开发领域的药物化学家的极大兴趣。组蛋白去乙酰化酶（HDAC）抑制剂是一类广泛的靶向抗癌药物。在探索的结构部分中，羟基苯甲酰胺和羟基丙烯酰胺已被证明具有潜在的 HDAC 抑制作用。这些结构类别中的几种化合物已被批准用于临床治疗不同类型的癌症，如伏立诺他和贝林司他。

目的

本研究旨在开发具有共轭喹唑啉酮骨架的新型 HDAC 抑制剂，具有针对不同癌细胞系的潜在细胞毒性。

方法

设计、合成并评价了一系列新型 N-羟基庚酰胺，其中包含共轭 6-羟基-2-甲基喹唑啉-4(3H)-酮（15a-l），用于 HDAC 抑制活性以及对三种人癌细胞系（HepG-2、MCF-7 和 SKLu-1）的细胞毒性。最后进行了分子模拟，以更深入地了解结构-活性关系。

结果

发现在所合成的新型共轭喹唑啉酮类羟肟酸中，化合物 15a、15c 和 15f 在 HDAC 抑制和细胞毒性方面最为有效。特别是化合物 15f 在 MCF-7 细胞系中的细胞毒性方面比 SAHA（伏立诺他）强近 4 倍，IC 值为 1.86 μM，HDAC 抑制的 IC 值为 6.36 μM。对 HDAC2 同工酶的对接实验表明，与 SAHA（-15.84 kcal/mol）相比，这些化合物与 HDAC2 的结合亲和力范围为-10.08 至-14.93 kcal/mol。在这项研究中还发现，大多数目标化合物似乎对 SKLu-1 的细胞毒性比对 MCF-7 和 HepG-2 的更强。