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Pharmacophore Modeling and in Silico/in Vitro Screening for Human Cytochrome P450 11B1 and Cytochrome P450 11B2 Inhibitors

机译:人类细胞色素P450 11B1和细胞色素P450 11B2抑制剂的药理学建模和计算机/体外筛选

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Cortisol synthase (CYP11B1) is the main enzyme for the endogenous synthesis of cortisol and its inhibition is a potential way for the treatment of diseases associated with increased cortisol levels, such as Cushing’s syndrome, metabolic diseases, and delayed wound healing. Aldosterone synthase (CYP11B2) is the key enzyme for aldosterone biosynthesis and its inhibition is a promising approach for the treatment of congestive heart failure, cardiac fibrosis, and certain forms of hypertension. Both CYP11B1 and CYP11B2 are structurally very similar and expressed in the adrenal cortex. To facilitate the identification of novel inhibitors of these enzymes, ligand-based pharmacophore models of CYP11B1 and CYP11B2 inhibition were developed. A virtual screening of the SPECS database was performed with our pharmacophore queries. Biological evaluation of the selected hits lead to the discovery of three potent novel inhibitors of both CYP11B1 and CYP11B2 in the submicromolar range (compounds 8-10), one selective CYP11B1 inhibitor (Compound 11, IC50 = 2.5 μM), and one selective CYP11B2 inhibitor (compound 12, IC50 = 1.1 μM), respectively. The overall success rate of this prospective virtual screening experiment is 20.8% indicating good predictive power of the pharmacophore models.
机译:皮质醇合成酶(CYP11B1)是皮质醇内源性合成的主要酶,其抑制作用是治疗与皮质醇水平升高相关的疾病的潜在方法,例如库欣综合征,代谢性疾病和伤口愈合延迟。醛固酮合酶(CYP11B2)是醛固酮生物合成的关键酶,其抑制作用是治疗充血性心力衰竭,心脏纤维化和某些形式的高血压的有前途的方法。 CYP11B1和CYP11B2在结构上非常相似,并在肾上腺皮质中表达。为促进这些酶的新型抑制剂的鉴定,开发了基于配体的CYP11B1和CYP11B2抑制作用的药效团模型。通过我们的药效团查询对SPECS数据库进行了虚拟筛选。对选定命中基因的生物学评估导致发现亚微摩尔范围内的三种有效的CYP11B1和CYP11B2新型抑制剂(化合物8-10),一种选择性CYP11B1抑制剂(化合物11,IC50 = 2.5μM)和一种选择性CYP11B2抑制剂(化合物12,IC50 = 1.1μM)。该前瞻性虚拟筛选实验的总体成功率为20.8%,表明药效基团模型具有良好的预测能力。

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