SYNTHESIS & PREDICTING THE POSSIBILITY OF 2, 5-DISUBSTITUTED-1, 3, 4-OXADIAZOLE DERIVATIVES AS GSK- 3? INHIBITORS

Shriram S. Purohit; V.P. Veerapur

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SYNTHESIS & PREDICTING THE POSSIBILITY OF 2, 5-DISUBSTITUTED-1, 3, 4-OXADIAZOLE DERIVATIVES AS GSK- 3? INHIBITORS

机译：合成并预测2、5-二取代-1、3、4-恶二唑衍生物作为GSK-3的可能性？抑制剂

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A new series of 2, 5-disubstituted-1, 3, 4-oxadiazole derivatives were synthesized using appropriate methods & structures of the synthesized compounds were confirmed by IR,NMR & Mass spectral data.. These ligands were prefiltered for their drug likeness properties by Lipinski's rule of 5 and it was found that all the ligands satisfied the rule of 5 for oral bioavailability.The prefiltered ligands were subjected for docking studies using integrated web server called docking server to investigate the interactions between the target compounds and the amino acid residues of the Glycogen synthase kinase-3|?. The docking studies were done using auto dock between computationally designed 2,5-disubstituted 1, 3, 4-oxadiazole derivatives and Glycogen synthase kinase-3beta (GSK-3|?) protein. The Calculated free energy of binding and estimated inhibition constants (Ki) were remarkable when compared with the standard GSK-3.inhibitors. It is calculated by the Lamarckian Genetic Algorithm (LGA). These values & the proposed interactions suggested that the 2, 5-disubstituted-1, 3, 4-oxadiazole derivatives are excellent inhibitors of GSK-3|?

机译：使用适当的方法合成了一系列新的2，5-二取代-1，3，4-恶二唑衍生物，并通过IR，NMR和质谱数据确定了合成化合物的结构。对这些配体的药物相似性进行了预过滤。根据Lipinski的5规则，发现所有配体均满足5的口服生物利用度规则。使用称为对接服务器的集成Web服务器对预过滤的配体进行对接研究，以研究目标化合物与氨基酸残基之间的相互作用糖原合酶激酶-3 |α的表达。对接研究是使用自动对接进行的，该对接是在计算设计的2，5-二取代的1、3、4-恶二唑衍生物与糖原合酶激酶3β（GSK-3 |β）蛋白之间进行的。与标准GSK-3抑制剂相比，结合自由能的计算值和估计的抑制常数（Ki）显着。它由Lamarckian遗传算法（LGA）计算。这些值和所提议的相互作用表明2，5-二取代-1，3，4-恶二唑衍生物是GSK-3 |β的优异抑制剂。

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《International Journal of Pharmaceutical Sciences and Research 》 |2012年第11期| 共9页
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Shriram S. Purohit; V.P. Veerapur;
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机译：含有杂环烷烃介晶基团的液晶聚合物。 5.含有2,5-二取代-1,3-二恶烷和2,5-二取代-1,3,2-二氧杂硼烷基中间介晶Gr的双相手性 - 近晶聚硅氧烷的合成

SYNTHESIS & PREDICTING THE POSSIBILITY OF 2, 5-DISUBSTITUTED-1, 3, 4-OXADIAZOLE DERIVATIVES AS GSK- 3? INHIBITORS

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