通过NCI数据库筛选寻找CDK-7激酶抑制剂的最新策略

IF 1 4区 化学 Q4 CHEMISTRY, MULTIDISCIPLINARY Journal of The Serbian Chemical Society Pub Date : 2023-01-01 DOI:10.2298/jsc230624083r
Mohammad Rashid, Md. Athar, Afzal Hussain, Norah Almadani, Ashfaq Hussain
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引用次数: 0

摘要

本研究基于对NCI数据库的探索,通过HTVS、SP、XP、分子对接、分子动力学模拟和ADMET评价等方法寻找特异性CDK-7激酶抑制剂。通过NCI数据库筛选筛选出最佳的CDK-7激酶抑制剂(NCI613391、NCI169676、NCI281246、NCI339580)。通过动力学模拟和MM-GBSA进一步证实了强效发现化合物(NCI613391)受体蛋白与蛋白配体复合物结合相互作用的稳定性。分析了受体和受体配体复合物的RMSD值,它揭示了结合相互作用的稳定性,并在整个模拟过程中保持稳定。未结合受体和主链原子的RMSF值和旋转半径相等,表明CDK7受体内的药物分子也是稳定的。MM-GBSA数据的研究还显示配体与CDK7受体的结合相互作用更强。除NCI169676外,所有化合物均为CYP450 2D6、CYP450 3A4、CYP450 2C9抑制剂和p糖蛋白非抑制剂的底物。根据Lipinski规则、Ghose过滤规则、MDDR样规则和cmc样规则,对所有化合物进行了药物相似性鉴定。该化合物(NCI613391)具有76.08%的人体肠道吸收率,AMES和T.E.S.T (US-EPA)阴性,具有OSIRIS特性,是一种很有前景的CDK-7激酶抑制剂,其疗效有待于进一步的临床研究。
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A recent tactic for searching CDK-7 kinase inhibitor by NCI database screening
The present study was based on an exploration of NCI database for searching specific CDK-7 kinase inhibitor by HTVS, SP, XP, molecular docking, molecular dynamic simulation, and ADMET evaluation. The best CDK-7 kinase inhibitors (NCI613391, NCI169676, NCI281246, NCI339580) were identified via NCI database screening. The stability of binding interaction between receptor protein and protein-ligand complex of potent finding compounds (NCI613391) further confirmed by dynamics simulations and MM-GBSA. The RMSD value of receptor and receptor-ligand complexes was analyzed, and it revealed the stability of binding interactions and remained stable throughout the simulation. The RMSF values and gyration radius of the unbound receptor and backbone atoms of the complex were found to be equal, which indicates that the drug molecule inside the CDK7 receptor is also stable. The study of MM-GBSA data also revealed stronger binding interactions of ligands to CDK7 receptors. With the exception of NCI169676, all compounds were shown to be substrates for CYP450 2D6, CYP450 3A4, inhibitors of CYP450 2C9, and non-inhibitors of p-glycoprotein. All compounds were qualified and found suitable to be as drug-likeness according to the Lipinski rule, Ghose filter, MDDR like rule, and CMC-like rule. The compound (NCI613391) was exhibited human intestinal absorption (76.08%), and display negative AMES and T.E.S.T (US-EPA) toxicity with OSIRIS property and found to be a promising CDK-7 kinase inhibitor and its efficacy may be further explored in clinical trials.
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来源期刊
CiteScore
1.80
自引率
0.00%
发文量
76
审稿时长
1 months
期刊介绍: The Journal of the Serbian Chemical Society -JSCS (formerly Glasnik Hemijskog društva Beograd) publishes articles original papers that have not been published previously, from the fields of fundamental and applied chemistry: Theoretical Chemistry, Organic Chemistry, Biochemistry and Biotechnology, Food Chemistry, Technology and Engineering, Inorganic Chemistry, Polymers, Analytical Chemistry, Physical Chemistry, Spectroscopy, Electrochemistry, Thermodynamics, Chemical Engineering, Textile Engineering, Materials, Ceramics, Metallurgy, Geochemistry, Environmental Chemistry, History of and Education in Chemistry.
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