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A novel central nervous system-penetrating protease inhibitor overcomes human immunodeficiency virus 1 resistance with unprecedented aM to pM potency

机译:一种新型的穿透中枢神经系统的蛋白酶抑制剂可克服人类免疫缺陷病毒1的耐药性并具有前所未有的aM到pM效能

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摘要

Antiretroviral therapy for HIV-1 infection/AIDS has significantly extended the life expectancy of HIV-1-infected individuals and reduced HIV-1 transmission at very high rates. However, certain individuals who initially achieve viral suppression to undetectable levels may eventually suffer treatment failure mainly due to adverse effects and the emergence of drug-resistant HIV-1 variants. Here, we report GRL-142, a novel HIV-1 protease inhibitor containing an unprecedented 6-5-5-ring-fused crown-like tetrahydropyranofuran, which has extremely potent activity against all HIV-1 strains examined with IC50 values of attomolar-to-picomolar concentrations, virtually no effects on cellular growth, extremely high genetic barrier against the emergence of drug-resistant variants, and favorable intracellular and central nervous system penetration. GRL-142 forms optimum polar, van der Waals, and halogen bond interactions with HIV-1 protease and strongly blocks protease dimerization, demonstrating that combined multiple optimizing elements significantly enhance molecular and atomic interactions with a target protein and generate unprecedentedly potent and practically favorable agents.
机译:针对HIV-1感染/艾滋病的抗逆转录病毒疗法显着延长了HIV-1感染者的预期寿命,并以很高的比率降低了HIV-1传播。但是,某些最初将病毒抑制到无法检测到的水平的个体最终可能会由于主要副作用和耐药性HIV-1变异体的出现而最终遭受治疗失败。在这里,我们报告了GRL-142,这是一种新型HIV-1蛋白酶抑制剂,它含有史无前例的6-5-5环稠合的冠状四氢吡喃呋喃,它对所有经attomolar-到皮摩尔浓度,对细胞生长几乎没有影响,对耐药变异出现的极高遗传屏障,以及良好的细胞内和中枢神经系统渗透能力。 GRL-142与HIV-1蛋白酶形成最佳的极性,范德华素和卤素键相互作用,并强烈阻断蛋白酶二聚化,表明结合多个优化元素可显着增强与靶蛋白的分子和原子相互作用,并产生前所未有的有效和实用的试剂。

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