首页> 美国卫生研究院文献>Pharmaceuticals >Chiral Derivatives of Xanthones: Investigation of the Effect of Enantioselectivity on Inhibition of Cyclooxygenases (COX-1 and COX-2) and Binding Interaction with Human Serum Albumin
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Chiral Derivatives of Xanthones: Investigation of the Effect of Enantioselectivity on Inhibition of Cyclooxygenases (COX-1 and COX-2) and Binding Interaction with Human Serum Albumin

机译:氧杂蒽酮的手性衍生物:对映选择性对环氧合酶(COX-1和COX-2)的抑制作用以及与人血清白蛋白结合相互作用的影响研究

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摘要

Searching of new enantiomerically pure chiral derivatives of xanthones (CDXs) with potential pharmacological properties, particularly those with anti-inflammatory activity, has remained an area of interest of our group. Herein, we describe in silico studies and in vitro inhibitory assays of cyclooxygenases (COX-1 and COX-2) for different enantiomeric pairs of CDXs. The evaluation of the inhibitory activities was performed by using the COX Inhibitor Screening Assay Kit. Docking simulations between the small molecules (CDXs; known ligands and decoys) and the enzyme targets were undertaken with AutoDock Vina embedded in PyRx—Virtual Screening Tool software. All the CDXs evaluated exhibited COX-1 and COX-2 inhibition potential as predicted. Considering that the (S)-(−)-enantiomer of the nonsteroidal anti-inflammatory drug ketoprofen preferentially binds to albumin, resulting in lower free plasma concentration than (R)-(+)-enantiomer, protein binding affinity for CDXs was also evaluated by spectrofluorimetry as well as in in silico. For some CDXs enantioselectivity was observed.
机译:寻找具有潜在药理特性,尤其是具有抗炎活性的新的对映体纯的手性黄原酮(CDXs)手性衍生物,仍然是我们研究的领域。在这里,我们描述了CDX的不同对映体对的计算机研究和环氧合酶(COX-1和COX-2)的体外抑制测定。通过使用COX抑制剂筛选测定试剂盒进行抑制活性的评估。小分子(CDXs;已知的配体和诱饵)与酶标靶之间的对接模拟是通过嵌入PyRx虚拟筛选工具软件中的AutoDock Vina进行的。评估的所有CDX均显示出预期的COX-1和COX-2抑制潜力。考虑到非甾体抗炎药酮洛芬的(S)-(-)-对映体优先与白蛋白结合,导致游离血浆浓度低于(R)-(+)-对映体,因此还评估了对CDXs的蛋白结合亲和力通过荧光分光光度法以及计算机分析。对于某些CDX,观察到对映选择性。

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