首页> 外文期刊>Journal of Medicinal Chemistry >Discovery of Chromane Containing Hepatitis C Virus (HCV) NS5A Inhibitors with Improved Potency against Resistance-Associated Variants
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Discovery of Chromane Containing Hepatitis C Virus (HCV) NS5A Inhibitors with Improved Potency against Resistance-Associated Variants

机译:发现具有增强的抗药性相关变体效力的含丙型肝炎病毒(HCV)NS5A抑制剂的铬烷。

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摘要

The discovery of potent and pan-genotypic HCV NSSA inhibitors faces many challenges including the significant diversity among genotypes, substantial potency shift conferred on some key resistance-associated variants, inconsistent SARs between different genotypes and mutants, and the lacking of models of inhibitor/protein complexes for rational inhibitor design. As part of ongoing efforts on HCV NSSA inhibition at Merck, we now describe the discovery of a novel series of chromane containing NSSA inhibitors. SAR studies around the "Z" group of the tetracyclic indole scaffold explored fused bicyclic rings as alternates to the phenyl group of elbasvir (1, MK-8742) and identified novel chromane and 2,3-dihydrobenzofuran derivatives as "Z" group replacements offered good potency across all genotypes. This effort, incorporating the C-1 fluoro substitution at the tetracyclic indole core, led to the discovery of a new series of NSSA inhibitors, such as compounds 14 and 25-28, with significantly improved potency against resistance-associated variants, such as GT2b, GT1a Y93H, and GT1a L31V. Compound 14 also showed reasonable PK exposures in preclinical species (rat and dog).
机译:高效和全基因型HCV NSSA抑制剂的发现面临许多挑战,包括基因型之间的显着差异,某些关键抗性相关变异赋予的显着效力变化,不同基因型和突变体之间的SAR不一致以及缺乏抑制剂/蛋白质模型的问题用于合理抑制剂设计的配合物。作为默克公司在抑制HCV NSSA方面正在进行的工作的一部分,我们现在描述发现一系列新的含苯并二氢吡喃的NSSA抑制剂的发现。 SAR研究围绕四环吲哚支架的“ Z”基团探索了稠合的双环作为Elbasvir(1,MK-8742)苯基的替代物,并确定了新的苯并二氢吡喃和2,3-二氢苯并呋喃衍生物作为“ Z”基团的替代品所有基因型均具有良好的效力。这项工作在四环吲哚核心处加入了C-1氟取代基,从而导致发现了一系列新的NSSA抑制剂,例如化合物14和25-28,其抗药性相关变体(例如GT2b)的效力大大提高。 ,GT1a Y93H和GT1a L31V。在临床前物种(大鼠和狗)中,化合物14还显示出合理的PK暴露。

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