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Development of an alphascreen-based HIV-1 integrase dimerization assay for discovery of novel allosteric inhibitors

机译:基于alpha筛选的HIV-1整合酶二聚化测定法的开发,用于发现新型变构抑制剂

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摘要

In recent years, HIV-1 integrase (IN) has become an established target in the field of antiretroviral drug discovery. However, its sole clinically approved inhibitor, the integrase strand transfer inhibitor (INSTI) raltegravir, has a surprisingly low genetic barrier for resistance. Furthermore, the only two other integrase inhibitors currently in advanced clinical trials, elvitegravir and dolutegravir, share its mechanism of action and certain resistance pathways. To maintain a range of treatment options, drug discovery efforts are now turning toward allosteric IN inhibitors, which should be devoid of cross-resistance with INSTIs. As IN requires a precise and dynamic equilibrium between several oligomeric species for its activities, the modulation of this equilibrium presents an interesting allosteric target. We report on the development, characterization, and validation of an AlphaScreen-based assay for high-throughput screening for modulators of HIV-1 IN dimerization. Compounds identified as hits in this assay proved to act as allosteric IN inhibitors. Additionally, the assay offers a flexible platform to study IN dimerization.
机译:近年来,HIV-1整合酶(IN)已成为抗逆转录病毒药物发现领域的既定目标。但是,其唯一的临床批准的抑制剂,整合酶链转移抑制剂(INSTI)raltegravir,具有令人惊讶的低耐药性遗传障碍。此外,目前在高级临床试验中,仅有的另外两种整合酶抑制剂elvitegravir和dolutegravir共享其作用机制和某些耐药途径。为了维持多种治疗选择,药物发现工作现在正在转向变构性IN抑制剂,该抑制剂应避免与INSTIs产生交叉耐药性。由于IN需要几种寡聚体之间进行精确而动态的平衡才能发挥其活性,因此该平衡的调节成为了一个有趣的变构靶标。我们报告开发,表征和验证的高通量筛选的HIV 1 IN二聚体调节剂的基于AlphaScreen的分析。在该测定法中被鉴定为命中的化合物被证明充当变构IN抑制剂。另外,该测定提供了研究IN二聚化的灵活平台。

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