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首页> 外文期刊>Scientific reports. >A Novel Assay for Screening Inhibitors Targeting HIV Integrase LEDGF/p75 Interaction Based on Ni2+ Coated Magnetic Agarose Beads
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A Novel Assay for Screening Inhibitors Targeting HIV Integrase LEDGF/p75 Interaction Based on Ni2+ Coated Magnetic Agarose Beads

机译:基于Ni2 +涂覆磁性琼脂糖珠筛选靶向HIV整体酶LEDGF / P75相互作用的筛选剂的新试验

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摘要

HIV-1 integrase (IN) plays an essential role in viral replication and thus serves as an important target for chemotherapeutic intervention against HIV-1 infection. However, the current three clinical IN inhibitors, raltegravir, elvitegravir and dolutegravir share the same inhibitory mechanism, resulting in a common clinical resistance profile which have emerged in infected patients receiving treatment. Therefore, it is important to develop small molecule inhibitors that impair IN function with distinct mechanisms of action. In this work, a magnetic-beads based biochemical assay targeting the protein-protein interaction (PPI) between HIV IN and the cellular cofactor LEDGF/p75 was developed for identification of HIV-1 IN inhibitors. Furthermore, a library containing 1000 US. Food and Drug Administration (FDA)-approved drugs currently used for human medication was screened to identify inhibitors targeting the PPI. The assay was proved to be quite robust and with the novel assay we successfully identified dexlansoprazole (IC50 of 4.8?μM), a FDA-approved proton pump inhibitor, as a potential inhibitor for the PPI between IN and LEDGF/p75, which bound to the LEDGF/p75 partner with a kinetic dissociation (Kd) constant of 330?nM?±?2.6?nM.
机译:HIV-1整合酶(IN)在病毒复制中起重要作用,因此是对HIV-1感染的化学治疗干预的重要目标。然而,目前在抑制剂中的三种临床,RALTEGRAVIR,ELVITEGRAVIR和DOLUTEGRAVIR共享相同的抑制机制,导致在受感染患者接受治疗的患者中出现的常见临床抗性曲线。因此,发展小分子抑制剂,以不同的作用机制损害功能。在这项工作中,开发了靶向蛋白质 - 蛋白质相互作用(PPI)和细胞辅因子LEDGF / P75之间的磁珠的生化测定,用于鉴定抑制剂中的HIV-1。此外,一个包含1000个美国的文库。筛选出目前用于人类药物的食品和药物管理局(FDA)批准药物以鉴定靶向PPI的抑制剂。被证明,测定是非常稳健的,并且具有新的测定,我们成功地鉴定了德克萨洛唑(IC50为4.8Ωμm),一种FDA批准的质子泵抑制剂,作为与...之间的PPI之间的潜在抑制剂,其结合在一起LEDGF / P75伴有动力解离(KD)常数为330?nm?±2.6?nm。

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