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3-Hydroxypyrimidine-24-dione-5-N-benzylcarboxamides potently inhibit HIV-1 integrase and RNase H

机译:3-羟基嘧啶-24-二酮-5-N-苄基羧酰胺有效抑制HIV-1整合酶和RNase H

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摘要

Resistance selection by human immunodeficiency virus (HIV) towards known drug regimens necessitates the discovery of structurally novel antivirals with a distinct resistance profile. Based on our previously reported 3-hydroxypyrimidine-2,4-dione (HPD) core we have designed and synthesized a new integrase strand transfer (INST) inhibitor type featuring a 5-N-benzylcarboxamide moiety. Significantly, the 6-alkylamino variant of this new chemotype consistently conferred low nanomolar inhibitory activity against HIV-1. Extended antiviral testing against a few raltegravir-resistant HIV-1 clones revealed a resistance profile similar to that of the second generation INST inhibitor (INSTIs) dolutegravir. Although biochemical testing and molecular modeling also strongly corroborate the inhibition of INST as the antiviral mechanism of action, selected antiviral analogues also potently inhibited reverse transcriptase (RT) associated RNase H, implying potential dual target inhibition. In vitro ADME assays demonstrated that this novel chemotype possesses largely favorable physicochemical properties suitable for further development.
机译:人类免疫缺陷病毒(HIV)对已知药物方案的耐药性选择必须发现具有独特耐药性的结构新颖的抗病毒药物。基于我们先前报道的3-hydroxypyrimidine-2,4-dione(HPD)核心,我们设计并合成了一种新型的整合酶链转移(INST)抑制剂类型,该抑制剂类型具有5-N-苄基羧酰胺部分。重要的是,这种新化学型的6-烷基氨基变体始终赋予针对HIV-1的低纳摩尔抑制活性。针对一些对拉格列韦耐药的HIV-1克隆的扩展抗病毒测试显示,其耐药性与第二代INST抑制剂(INSTIs)dolutegravir类似。尽管生化测试和分子建模也强烈证实了INST作为抗病毒作用机制的抑制作用,但所选的抗病毒类似物也有效抑制了逆转录酶(RT)相关的RNase H,暗示了潜在的双重靶标抑制作用。体外ADME分析表明,这种新的化学型具有非常有利的理化性质,适合进一步开发。

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