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Novel 2-Substituted 7-Azaindole and7-Azaindazole Analogues as Potential Antiviral Agents for theTreatment of Influenza

机译:新型2取代7-氮杂吲哚和7-氮杂吲唑类似物作为潜在的抗病毒药物流感的治疗

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摘要

JNJ-63623872 (>2) is a first-in-class, orally bioavailable compound that offers significant potential for the treatment of pandemic and seasonal influenza. Early lead optimization efforts in our 7-azaindole series focused on 1,3-diaminocyclohexyl amide and urea substitutions on the pyrimidine-7-azaindole motif. In this work, we explored two strategies to eliminate observed aldehyde oxidase (AO)-mediated metabolism at the 2-position of these 7-azaindole analogues. Substitution at the 2-position of the azaindole ring generated somewhat less potent analogues, but reduced AO-mediated metabolism. Incorporation of a ring nitrogen generated 7-azaindazole analogues that were equipotent to the parent 2-H-7-azaindole, but surprisingly, did not appear to improve AO-mediated metabolism. Overall, we identified multiple 2-substituted 7-azaindole analogues with enhanced AO stability and we present data for one such compound (>12) that demonstrate a favorable oral pharmacokinetic profile in rodents. These analogues have the potential to be further developed as anti-influenza agents for the treatment of influenza.
机译:JNJ-63623872(> 2 )是一流的,口服可生物利用的化合物,为大流行和季节性流感的治疗提供了巨大的潜力。在我们的7-氮杂吲哚系列中,早期的铅优化工作集中在嘧啶-7-氮杂吲哚基序上的1,3-二氨基环己基酰胺和尿素取代上。在这项工作中,我们探索了两种消除在这些7-氮杂吲哚类似物的2位上观察到的醛氧化酶(AO)介导的代谢的策略。在氮杂吲哚环的2-位取代产生了效力稍弱的类似物,但是减少了AO介导的代谢。环氮的引入产生了与母体2-H-7-氮杂吲哚等价的7-氮杂吲唑类似物,但是令人惊讶地,似乎没有改善AO介导的代谢。总的来说,我们鉴定了多个具有增强的AO稳定性的2-取代的7-氮杂吲哚类似物,并且我们提供了一种此类化合物(> 12 )的数据,这些化合物在啮齿动物中具有良好的口服药代动力学特征。这些类似物有可能被进一步开发为用于治疗流感的抗流感药物。

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