{"title":"基于计算机筛选和进一步体外验证的新型GABA阳性变构调节剂鉴定集成工作流程。使用Enamine的库存化学空间进行案例研究。","authors":"Maksym Platonov, Oleksandr Maximyuk, Alexey Rayevsky, Olena Iegorova, Vasyl Hurmach, Yuliia Holota, Elijah Bulgakov, Andrii Cherninskyi, Pavel Karpov, Sergey Ryabukhin, Oleg Krishtal, Dmitriy Volochnyuk","doi":"10.1002/minf.202300156","DOIUrl":null,"url":null,"abstract":"<p><p>Numerous studies reported an association between GABA<sub>A</sub> R subunit genes and epilepsy, eating disorders, autism spectrum disorders, neurodevelopmental disorders, and bipolar disorders. This study was aimed to find some potential positive allosteric modulators and was performed by combining the in silico approach with further in vitro evaluation of its real activity. We started from the GABA<sub>A</sub> R-diazepam complexes and assembled a lipid embedded protein ensemble to refine it via molecular dynamics (MD) simulation. Then we focused on the interaction of α1β2γ2 with some Z-drugs (non-benzodiazepine compounds) using an Induced Fit Docking (IFD) into the relaxed binding site to generate a pharmacophore model. The pharmacophore model was validated with a reference set and applied to decrease the pre-filtered Enamine database before the main docking procedure. Finally, we succeeded in identifying a set of compounds, which met all features of the docking model. The aqueous solubility and stability of these compounds in mouse plasma were assessed. Then they were tested for the biological activity using the rat Purkinje neurons and CHO cells with heterologously expressed human α1β2γ2 GABA<sub>A</sub> receptors. Whole-cell patch clamp recordings were used to reveal the GABA induced currents. Our study represents a convenient and tunable model for the discovery of novel positive allosteric modulators of GABA<sub>A</sub> receptors. 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引用次数: 0
摘要
大量研究报道了GABA - AR亚基基因与癫痫、饮食失调、自闭症谱系障碍、神经发育障碍和双相情感障碍之间的关联。本研究旨在寻找一些潜在的正变构调节剂,并将计算机方法与进一步的体外活性评估相结合。我们从GABA - ar -地西泮复合物开始,通过分子动力学(MD)模拟组装了一个脂质嵌入蛋白集合来完善它。然后,我们将重点放在α1β2γ2与一些z -药物(非苯二氮卓类化合物)的相互作用上,利用诱导匹配对接(IFD)进入松弛结合位点,产生药效团模型。利用参考集验证药效团模型,并在主对接前减少预过滤的Enamine数据库。最后,我们成功地鉴定出一组符合对接模型所有特征的化合物。评估了这些化合物在小鼠血浆中的水溶性和稳定性。然后用大鼠浦肯野神经元和异源表达人α1β2γ2 GABAA受体的CHO细胞检测其生物活性。全细胞膜片钳记录显示GABA诱导电流。我们的研究为发现GABAA受体的新型正变构调节剂提供了一个方便和可调的模型。对最大的可用化合物数据库进行高通量虚拟筛选,筛选出23种化合物。进一步的电生理测试使我们确定了一组3个最突出的活性化合物。考虑到先导化合物的结构特点,该研究可以很快发展为MedChem项目。
Integrated workflow for the identification of new GABAA R positive allosteric modulators based on the in silico screening with further in vitro validation. Case study using Enamine's stock chemical space.
Numerous studies reported an association between GABAA R subunit genes and epilepsy, eating disorders, autism spectrum disorders, neurodevelopmental disorders, and bipolar disorders. This study was aimed to find some potential positive allosteric modulators and was performed by combining the in silico approach with further in vitro evaluation of its real activity. We started from the GABAA R-diazepam complexes and assembled a lipid embedded protein ensemble to refine it via molecular dynamics (MD) simulation. Then we focused on the interaction of α1β2γ2 with some Z-drugs (non-benzodiazepine compounds) using an Induced Fit Docking (IFD) into the relaxed binding site to generate a pharmacophore model. The pharmacophore model was validated with a reference set and applied to decrease the pre-filtered Enamine database before the main docking procedure. Finally, we succeeded in identifying a set of compounds, which met all features of the docking model. The aqueous solubility and stability of these compounds in mouse plasma were assessed. Then they were tested for the biological activity using the rat Purkinje neurons and CHO cells with heterologously expressed human α1β2γ2 GABAA receptors. Whole-cell patch clamp recordings were used to reveal the GABA induced currents. Our study represents a convenient and tunable model for the discovery of novel positive allosteric modulators of GABAA receptors. A High-throughput virtual screening of the largest available database of chemical compounds resulted in the selection of 23 compounds. Further electrophysiological tests allowed us to determine a set of 3 the most outstanding active compounds. Considering the structural features of leader compounds, the study can develop into the MedChem project soon.
期刊介绍:
Molecular Informatics is a peer-reviewed, international forum for publication of high-quality, interdisciplinary research on all molecular aspects of bio/cheminformatics and computer-assisted molecular design. Molecular Informatics succeeded QSAR & Combinatorial Science in 2010.
Molecular Informatics presents methodological innovations that will lead to a deeper understanding of ligand-receptor interactions, macromolecular complexes, molecular networks, design concepts and processes that demonstrate how ideas and design concepts lead to molecules with a desired structure or function, preferably including experimental validation.
The journal''s scope includes but is not limited to the fields of drug discovery and chemical biology, protein and nucleic acid engineering and design, the design of nanomolecular structures, strategies for modeling of macromolecular assemblies, molecular networks and systems, pharmaco- and chemogenomics, computer-assisted screening strategies, as well as novel technologies for the de novo design of biologically active molecules. As a unique feature Molecular Informatics publishes so-called "Methods Corner" review-type articles which feature important technological concepts and advances within the scope of the journal.