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新型普乐可复衍生物:异噁唑环和苯环取代基对肠道病毒抗病毒活性的影响。

Novel pleconaril derivatives: Influence of substituents in the isoxazole and phenyl rings on the antiviral activity against enteroviruses.

机构信息

Bach Institute of Biochemistry, Research Center of Biotechnology of the Russian Academy of Sciences, 33-2 Leninsky Prospect, Moscow, 119071, Russia.

Jena University Hospital, Department of Medical Microbiology, Section Experimental Virology, Hans-Knöll-Strasse 2, Jena, 07745, Germany.

出版信息

Eur J Med Chem. 2020 Feb 15;188:112007. doi: 10.1016/j.ejmech.2019.112007. Epub 2019 Dec 23.

Abstract

Today, there are no medicines to treat enterovirus and rhinovirus infections. In the present study, a series of novel pleconaril derivatives with substitutions in the isoxazole and phenyl rings was synthesized and evaluated for their antiviral activity against a panel of pleconaril-sensitive and -resistant enteroviruses. Studies of the structure-activity relationship demonstrate the crucial role of the N,N-dimethylcarbamoyl group in the isoxazole ring for antiviral activity against pleconaril-resistant viruses. In addition, one or two substituents in the phenyl ring directly impact on the spectrum of antienteroviral activity. The 3-(3-methyl-4-(3-(3-N,N-dimethylcarbamoyl-isoxazol-5-yl)propoxy)phenyl)-5-trifluoromethyl-1,2,4-oxadiazole 10g was among the compounds exhibiting the strongest activity against pleconaril-resistant as well as pleconaril-susceptible enteroviruses with IC values from 0.02 to 5.25 μM in this series. Compound 10g demonstrated markedly less CYP3A4 induction than pleconaril, was non-mutagenic, and was bioavailable after intragastric administration in mice. These results highlight compound 10g as a promising potential candidate as a broad spectrum enterovirus and rhinovirus inhibitor for further preclinical investigations.

摘要

目前尚无治疗肠道病毒和鼻病毒感染的药物。在本研究中,我们合成了一系列异噁唑环和苯环取代的新型吡喃那韦衍生物,并评估了它们对一系列吡喃那韦敏感和耐药肠道病毒的抗病毒活性。结构-活性关系研究表明,异噁唑环中的 N,N-二甲基氨基甲酰基对于抗吡喃那韦耐药病毒的活性至关重要。此外,苯环中的一个或两个取代基直接影响抗肠道病毒活性的范围。在该系列化合物中,3-(3-甲基-4-(3-(3-N,N-二甲基氨基甲酰基-异噁唑-5-基)丙氧基)苯基)-5-三氟甲基-1,2,4-噁二唑 10g 对吡喃那韦耐药和敏感的肠道病毒均具有最强的活性,其对肠道病毒的 IC 值为 0.02 至 5.25 μM。与吡喃那韦相比,化合物 10g 对 CYP3A4 的诱导作用明显减弱,无致突变性,并且在小鼠胃内给药后具有生物利用度。这些结果突出了化合物 10g 作为一种有前途的广谱肠道病毒和鼻病毒抑制剂的潜在候选药物,值得进一步进行临床前研究。

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