Gamba Elia, Mori Mattia, Kovalenko Lesia, Giannini Alessia, Sosic Alice, Saladini Francesco, Fabris Dan, Mély Yves, Gatto Barbara, Botta Maurizio
Dipartimento di Scienze del Farmaco, Università di Padova, via Marzolo 5, 35131 Padova, Italy.
Dipartimento di Biotecnologie, Chimica e Farmacia, Università degli Studi di Siena, via A. Moro, 53100 Siena, Italy.
Eur J Med Chem. 2018 Feb 10;145:154-164. doi: 10.1016/j.ejmech.2017.12.073. Epub 2017 Dec 24.
In this report, we present a new benzoxazole derivative endowed with inhibitory activity against the HIV-1 nucleocapsid protein (NC). NC is a 55-residue basic protein with nucleic acid chaperone properties, which has emerged as a novel and potential pharmacological target against HIV-1. In the pursuit of novel NC-inhibitor chemotypes, we performed virtual screening and in vitro biological evaluation of a large library of chemical entities. We found that compounds sharing a benzoxazolinone moiety displayed putative inhibitory properties, which we further investigated by considering a series of chemical analogues. This approach provided valuable information on the structure-activity relationships of these compounds and, in the process, demonstrated that their anti-NC activity could be finely tuned by the addition of specific substituents to the initial benzoxazolinone scaffold. This study represents the starting point for the possible development of a new class of antiretroviral agents targeting the HIV-1 NC protein.
在本报告中,我们展示了一种新型苯并恶唑衍生物,其对HIV-1核衣壳蛋白(NC)具有抑制活性。NC是一种具有55个残基的碱性蛋白,具有核酸伴侣特性,已成为针对HIV-1的新型潜在药理学靶点。为了寻找新型NC抑制剂化学类型,我们对大量化学实体库进行了虚拟筛选和体外生物学评估。我们发现,具有苯并恶唑啉酮部分的化合物表现出假定的抑制特性,我们通过考虑一系列化学类似物对其进行了进一步研究。这种方法提供了有关这些化合物构效关系的有价值信息,并且在此过程中证明,通过在初始苯并恶唑啉酮支架上添加特定取代基,可以精细调节它们的抗NC活性。这项研究代表了可能开发一类针对HIV-1 NC蛋白的新型抗逆转录病毒药物的起点。
