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Pharmacophore Mapping and Virtual Screening for SIRT1 Activators

机译:SIRT1激活剂的药理映射和虚拟筛选

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Silent information regulator 2 (Sir2) or sirtuins are NAD(+)-dependent deacetylases, which hydrolyze the acetyl-lysine residues. In mammals, sirtuins are classified into seven different classes (SIRT1-7). SIRT1 was reported to be involved in age related disorders like obesity, metabolic syndrome, type II diabetes mellitus and Parkinson's disease. Activation of SIRT1 is one of the promising approaches to treat these age related diseases. In this study, we have used HipHop module of CATALYST to identify a series of pharmacophore models to screen SIRT1 enhancing molecules. Three molecules from Sirtris Pharmaceuticals were selected as training set and 607 sirtuin activator molecules were used as test set. Five different hypotheses were developed and then validated using the training set and the test set. The results showed that the best pharmacophore model has four features, ring aromatic, positive ionization and two hydrogen-bond acceptors. The best hypothesis from our study, Hypo2, screened high number of active molecules from the test set. Thus, we suggest that this four feature pharmacophore model could be helpful to screen novel SIRT1 activator molecules. Hypo2-virtual screening against Maybridge database reveals seven molecules, which contains all the critical features. Moreover, two new scaffolds were identified from this study. These scaffolds may be a potent lead for the SIRT1 activation.
机译:沉默信息调节剂2(Sir2)或sirtuins是NAD(+)依赖性脱乙酰基酶,可水解乙酰赖氨酸残基。在哺乳动物中,沉默调节蛋白被分为七个不同的类别(SIRT1-7)。据报道,SIRT1参与了与年龄有关的疾病,例如肥胖,代谢综合征,II型糖尿病和帕金森氏病。 SIRT1的激活是治疗这些年龄相关疾病的有前途的方法之一。在这项研究中,我们使用了CATALYST的HipHop模块来识别一系列药效团模型来筛选SIRT1增强分子。选择来自Sirtris Pharmaceuticals的三个分子作为训练集,并使用607个沉默调节蛋白的活化剂分子作为测试集。建立了五个不同的假设,然后使用训练集和测试集进行了验证。结果表明,最佳药效团模型具有四个特征:环芳烃,正电离和两个氢键受体。我们研究中最好的假设Hypo2从测试集中筛选出大量活性分子。因此,我们建议这四个功能的药效团模型可能有助于筛选新型SIRT1激活分子。根据Maybridge数据库进行的次二病毒筛选显示出七个分子,其中包含所有关键特征。此外,从该研究中鉴定出两个新的支架。这些支架可能是SIRT1激活的有效线索。

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