Design, synthesis, and anti-TMV bioactivities of nucleobase phosphonate analogs

Zhenxing Li, He-Shu Fang, Wubin Shao, Peiyi Wang, Zhi-bing Wu, Song Yang
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引用次数: 5

Abstract

GRAPHICAL ABSTRACT ABSTRACT A series of novel nucleobase derivatives and their analogues possessing diethoxyphosphoryl scaffolds were synthesized through four-step reactions and screened for their antiviral activity toward tobacco mosaic virus (TMV). Preliminary bioassays suggested that some of these simple structures displayed appreciable anti-TMV activity in vivo. Among them, compound (diethoxyphosphoryl)methyl 4-[2-(1H-benzo[d][1,2,3]triazol-1-yl)acetamido]-benzoate (a-3) exerted the strongest chemotherapeutic and protective effects against TMV with the rates of 52.8 and 72.2% at the dosage of 500 µg/mL, respectively, which were comparable with those of the commercial agricultural antiviral agent ningnanmycin (54.2 and 70.2%). Molecular docking with TMV helicases revealed that compound a-3 had strong interactions with receptor amino acid residues. Given the facile synthetic route and significant chemotherapeutic and protective potentials, compound a-3 could be further studied and exploited as a promising antiviral candidate.
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膦酸核碱基类似物的设计、合成及抗tmv生物活性
摘要/ ABSTRACT通过四步反应合成了一系列具有二氧磷基支架的新型核碱基衍生物及其类似物,并对其抗烟草花叶病毒(TMV)的活性进行了筛选。初步的生物测定表明,其中一些简单的结构在体内表现出明显的抗tmv活性。其中,化合物(二氧磷酰基)甲基4-[2-(1h -苯并[d][1,2,3]三唑-1-酰基)乙酰氨基]-苯甲酸酯(a-3)对TMV的化疗和保护作用最强,在500µg/mL剂量下分别为52.8和72.2%,与市售农用抗病毒药物宁南霉素(54.2和70.2%)相当。与TMV解旋酶的分子对接表明,化合物a-3与受体氨基酸残基有很强的相互作用。鉴于化合物a-3的合成路线简单,具有显著的化疗和保护作用,因此可以作为一种有前景的抗病毒候选药物进行进一步研究和开发。
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