Molecular docking studies on tetrahydroimidazo-[4,5,1-jk][1,4]-benzodiazepinone (TIBO) derivatives as HIV-1NNRT inhibitors

Sapre NS; Gupta S; Pancholi N; Sapre N

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Molecular docking studies on tetrahydroimidazo-[4,5,1-jk][1,4]-benzodiazepinone (TIBO) derivatives as HIV-1NNRT inhibitors

机译：四氢咪唑-[4,5,1-jk] [1,4]-苯并二氮杂酮（TIBO）衍生物作为HIV-1NNRT抑制剂的分子对接研究

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At present, chemotherapy seems to be the main weapon in the arsenal of remedies for the ongoing crusade against AIDS. The mode of binding of the TIBO family of inhibitors has been of interest because these compounds do not fit the two-hinged-ring model as generally observed in the NNRTIs. Flexible docking simulations were performed with a series of 53 TIBO derivatives as NNRTIs. Binding preferences as well as the structural and energetic factors associated with them were studied. A good correlation (r(2) = 0.849, q(2) = 0.843) was observed between the biological activity and binding affinity of the compounds which suggest that the identified binding conformations of these inhibitors are reliable. Further screening of PubChem database yielded novel scaffolds. Our studies suggest that modifications to the TIBO group of inhibitors might enhance their binding efficacy and hence, potentially, their therapeutic utility.

机译：目前，化学疗法似乎是正在进行的抗击艾滋病斗争的主要手段。 TIBO抑制剂家族的结合方式引起了人们的兴趣，因为这些化合物不适合NNRTIs中通常观察到的双环模型。使用一系列53种TIBO衍生物作为NNRTIs进行灵活的对接模拟。研究了结合偏好以及与之相关的结构和能量因素。在化合物的生物学活性和结合亲和力之间观察到良好的相关性（r（2）= 0.849，q（2）= 0.843），这表明这些抑制剂的确定结合构象是可靠的。进一步筛选PubChem数据库可得到新型支架。我们的研究表明，对TIBO抑制剂组的修饰可能会增强其结合功效，因此可能会提高其治疗效用。

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《Journal of Computer-Aided Molecular Design》 |2008年第2期|共12页
作者
Sapre NS; Gupta S; Pancholi N; Sapre N;
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正文语种 eng
中图分类物理化学（理论化学）、化学物理学;
关键词
TIBO; structure based drug design (SBDD); HIV-1 non-nucleoside reverse transcriptase inhibitors (HIV-1 NNRTIs); pIC(50); multiple linear regression (MLR); artificial neural network (ANN); REVERSE-TRANSCRIPTASE INHIBITORS; RT NONNUCLEOSIDE INHIBITORS; ANTIRETROVIRAL THERAPY; INFECTED PATIENTS; WILD-TYPE; COMPLEX; BINDING; RESOLUTION; DESIGN; RESISTANCE;

机译：TIBO;基于结构的药物设计（SBDD）;HIV-1非核苷逆转录酶抑制剂（HIV-1 NNRTIs）;pIC（50）;多元线性回归（MLR）;人工神经网络（ANN）;逆转录酶抑制剂;RT核苷类抑制剂;抗玻璃体治疗;感染患者;野生型;络合物;结合;拆分;设计;耐药;

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1. Molecular docking studies on tetrahydroimidazo-[4,5,1-jk][1,4]-benzodiazepinone (TIBO) derivatives as HIV-1NNRT inhibitors [J] . Sapre NS, Gupta S, Pancholi N, Journal of Computer-Aided Molecular Design . 2008,第2期

机译：四氢咪唑-[4,5,1-jk] [1,4]-苯并二氮杂酮（TIBO）衍生物作为HIV-1NNRT抑制剂的分子对接研究
2. Data mining using template-based molecular docking on tetrahydroimidazo-[4,5,1-jk][1,4]-benzodiazepinone (TIBO) derivatives as HIV-1RT inhibitors [J] . Sapre NS, Gupta S, Pancholi N, Journal of molecular modeling . 2008,第11期

机译：使用基于模板的分子对接作为HIV-1RT抑制剂的四氢咪唑-[4,5,1-jk] [1,4]-苯并二氮杂酮（TIBO）衍生物进行数据挖掘
3. Data mining using template-based molecular docking on tetrahydroimidazo-[4,5,1-jk][1,4]-benzodiazepinone (TIBO) derivatives as HIV-1RT inhibitors [J] . Nitin S. Sapre, Swagata Gupta, Nilanjana Pancholi, Journal of Molecular Modeling . 2008,第11期

机译：使用基于模板的分子对接作为HIV-1RT抑制剂的四氢咪唑-[4,5,1-jk] [1,4]-苯并二氮杂酮（TIBO）衍生物进行数据挖掘
4. Molecular Docking Analysis of Podophyllotoxin Derivatives in Sulawesi Propolis as Potent Inhibitors of Protein Kinases [C] . Darin Flamandita, Kenny Lischer, Diah Kartika Pratami, International Symposium on Sustainable and Clean Energy;International Conference on Quality in Research . 2020

机译：洛叶葡萄球菌毒素衍生物的分子对接分析蛋白酶激酶有效抑制剂
5. A. Studies towards the formation of asymmetric quaternary centres via radical allylation. B. Applications of chiral hydrazide organocatalysts to Diels-Alder, hydride reduction, and alpha-chlorination reactions. C. Studies directed towards the synthesis of potential HIV-1 reverse transcriptase inhibitors: 9-Alkylaryl TIBO derivatives. [D] . Aumand, Livia M. 2005

机译：A.关于通过自由基烯丙基化形成不对称四元中心的研究。 B.手性酰肼有机催化剂在Diels-Alder，氢化物还原和α-氯化反应中的应用。 C.针对潜在的HIV-1逆转录酶抑制剂的合成的研究：9-烷基芳基TIBO衍生物。
6. 2D-QSAR and docking study of a series of coumarin derivatives as inhibitors of CDK (anticancer activity) with an application of the molecular docking method [O] . Rania Kasmi, Elghalia Hadaji, Oussama Chedadi, 2020

机译：2D-QSAR和对接研究一系列香豆素衍生物作为CDK（抗癌活性）的抑制剂应用分子对接方法
7. Assessing ligand efficiencies using template-based molecular docking and Tabu-clustering on tetrahydroimidazo-4,5,1-jk1,4-benzodiazepin-2(1H)-one and-thione (TIBO) derivatives as HIV-1RT inhibitors [O] . Nitin S. Sapre, Swagata Gupta, Neelima Sapre 2008

机译：评估使用基于模板的分子对接和虎图聚类的配体效率，并在四氢咪唑 - 4,5,1-JK 1,4 - 苯并二氮嘧啶-2（1H） - 酮（Tibo）衍生物作为HIV-1RT抑制剂

Molecular docking studies on tetrahydroimidazo-[4,5,1-jk][1,4]-benzodiazepinone (TIBO) derivatives as HIV-1NNRT inhibitors

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