Synthesis, Structure-Activity Relationships, and Antiviral Activity of Allosteric Inhibitors of Flavivirus NS2B-NS3 Protease

Nie Shenyou; Yao Yuan; Wu Fangrui; Wu Xiaowei; Zhao Jidong; Hua Yuanda; Wu Jingyu; Huo Tong; Lin Yi-Lun; Kneubehl Alexander R.; Vogt Megan B.; Ferreon Josephine; Rico-Hesse Rebecca; Song Yongcheng

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Synthesis, Structure-Activity Relationships, and Antiviral Activity of Allosteric Inhibitors of Flavivirus NS2B-NS3 Protease

机译：黄病毒NS2B-NS3蛋白酶变构抑制剂的合成，结构活性关系和抗病毒活性

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Flaviviruses, including Zika, dengue, and West Nile viruses, are important human pathogens. The highly conserved NS2B-NS3 protease of Flavivirus is essential for viral replication and therefore a promising drug target. Through compound screening, followed by medicinal chemistry studies, a novel series of 2,5,6-trisubstituted pyrazine compounds are found to be potent, allosteric inhibitors of Zika virus protease (ZVpro) with IC50 values as low as 130 nM. Their structure-activity relationships are discussed. The ZVpro inhibitors also inhibit homologous proteases of dengue and West Nile viruses, and their inhibitory activities are correlated. The most potent compounds 47 and 103 potently inhibited Zika virus replication in cells with EC68 values of 300-600 nM and in a mouse model of Zika infection. These compounds represent novel pharmacological leads for drug development against Flavivirus infections.

机译：包括寨卡病毒、登革热病毒和西尼罗河病毒在内的黄病毒是重要的人类病原体。黄病毒高度保守的NS2B-NS3蛋白酶对病毒复制至关重要，因此是一个有前途的药物靶点。通过化合物筛选，然后进行药物化学研究，发现一系列新的2,5,6-三取代吡嗪化合物是寨卡病毒蛋白酶（ZVpro）的有效变构抑制剂，IC50值低至130 nM。讨论了它们的构效关系。ZVpro抑制剂还抑制登革热和西尼罗河病毒的同源蛋白酶，并且它们的抑制活性是相关的。最有效的化合物47和103在EC68值为300-600 nM的细胞和寨卡感染小鼠模型中有效抑制寨卡病毒复制。这些化合物代表了抗黄病毒感染药物开发的新药理学线索。

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来源
《Journal of Medicinal Chemistry 》 |2021年第5期| 共24页
作者
Nie Shenyou; Yao Yuan; Wu Fangrui; Wu Xiaowei; Zhao Jidong; Hua Yuanda; Wu Jingyu; Huo Tong; Lin Yi-Lun; Kneubehl Alexander R.; Vogt Megan B.; Ferreon Josephine; Rico-Hesse Rebecca; Song Yongcheng;
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作者单位

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Mol Virol &

Microbiol Houston TX 77030 USA;

Baylor Coll Med Dept Mol Virol &

Microbiol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

Baylor Coll Med Dept Mol Virol &

Microbiol Houston TX 77030 USA;

Baylor Coll Med Dept Pharmacol &

Chem Biol Houston TX 77030 USA;

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正文语种 eng
中图分类药学 ;
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4. Discovery, X-ray Crystallography and Antiviral Activity of Allosteric Inhibitors of Flavivirus NS2B-NS3 Protease [J] . Yao Yuan, Huo Tong, Lin Yi-Lun, Journal of the American Chemical Society . 2019 ,第17期

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Synthesis, Structure-Activity Relationships, and Antiviral Activity of Allosteric Inhibitors of Flavivirus NS2B-NS3 Protease

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