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作为有效的泛丝状病毒抑制剂的雌激素受体配体的筛选和反向工程。

Screening and Reverse-Engineering of Estrogen Receptor Ligands as Potent Pan-Filovirus Inhibitors.

机构信息

Department of Pharmaceutical Sciences, College of Pharmacy, and UICentre, University of Illinois at Chicago, Chicago, Illinois 60612, United States.

Department of Microbiology and Immunology, College of Medicine, University of Illinois at Chicago, Chicago, Illinois 60612, United States.

出版信息

J Med Chem. 2020 Oct 8;63(19):11085-11099. doi: 10.1021/acs.jmedchem.0c01001. Epub 2020 Sep 22.

Abstract

Filoviridae, including Ebola (EBOV) and Marburg (MARV) viruses, are emerging pathogens that pose a serious threat to public health. No agents have been approved to treat filovirus infections, representing a major unmet medical need. The selective estrogen receptor modulator (SERM) toremifene was previously identified from a screen of FDA-approved drugs as a potent EBOV viral entry inhibitor, via binding to EBOV glycoprotein (GP). A focused screen of ER ligands identified ridaifen-B as a potent dual inhibitor of EBOV and MARV. Optimization and reverse-engineering to remove ER activity led to a novel compound () showing potent inhibition against infectious EBOV Zaire (0.09 μM) and MARV (0.64 μM). Mutagenesis studies confirmed that inhibition of EBOV viral entry is mediated by the direct interaction with GP. Importantly, compound displayed a broad-spectrum antifilovirus activity against Bundibugyo, Tai Forest, Reston, and Měnglà viruses and is the first submicromolar antiviral agent reported for some of these strains, therefore warranting further development as a pan-filovirus inhibitor.

摘要

丝状病毒科包括埃博拉病毒(EBOV)和马尔堡病毒(MARV),是对公共卫生构成严重威胁的新兴病原体。目前尚无药物被批准用于治疗丝状病毒感染,这是一个未满足的主要医疗需求。先前从 FDA 批准的药物筛选中发现选择性雌激素受体调节剂(SERM)托瑞米芬是一种有效的埃博拉病毒进入抑制剂,通过与埃博拉病毒糖蛋白(GP)结合。对 ER 配体的针对性筛选发现瑞达芬-B 是一种有效的埃博拉病毒和马尔堡病毒双重抑制剂。对 ER 活性进行优化和反向工程得到了一种新型化合物(),对感染性扎伊尔埃博拉病毒(0.09 μM)和马尔堡病毒(0.64 μM)具有很强的抑制作用。突变研究证实,埃博拉病毒进入的抑制是由与 GP 的直接相互作用介导的。重要的是,化合物对 Bundibugyo、Tai Forest、Reston 和 Menglà 病毒均显示出广谱抗丝状病毒活性,并且是针对其中一些毒株的第一个亚毫摩尔抗病毒药物,因此有理由进一步将其开发为泛丝状病毒抑制剂。

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