Quinazolines as inhibitors of chromatin-associated proteins in histones

被引:0
|
作者
Frida S. Herrera-Vázquez
Francisco Hernández-Luis
José L. Medina Franco
机构
[1] Universidad Nacional Autónoma de México,Facultad de Química, Departamento de Farmacia
来源
Medicinal Chemistry Research | 2019年 / 28卷
关键词
Quinazoline chromatin-associated proteins; Epigenetic; Histone modifiers; Inhibitors;
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摘要
It is increasing the evidence that quinazolines are inhibitors of chromatin-associated proteins in histones. Quinazolines have a broad structural diversity among the structural classes that have been designed. Herein, we review the development of selective and potent quinazolines highlighting the current state of these molecules with an emphasis on the structural requirements for the interaction within the target. Chemical synthesis and results of the biological assays in vitro or in vivo of these compounds are also discussed. There is extensive evidence that support quinazoline derivatives as inhibitors of histone methyltransferase (G9a) and G9a-like protein (GLP). There is one quinazoline analogue that inhibits an extra-terminal bromodomain motif (BET) and that is on clinical trials as potential treatment for different chronic diseases. There is also clinical evidence that quinazolines act as dual inhibitors targeting histone deacetylases (HDACs) Zn2+-dependent and kinase receptors for the potential treatment of cancer. Additional proposals of quinazoline structures are being evaluated as inhibitors targeting two or more chromatin-associated proteins simultaneously. Therefore, further improvements in synthetic methods, computational studies, and additional biological assays in vitro and in vivo remain to be addressed.
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页码:395 / 416
页数:21
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