In vivo antiviral activity and disassembly mechanism of novel 1-phe- nyl-5-amine-4-pyrazole thioether derivatives against Tobacco mosaic virus

被引:33
作者
Wu, Zhibing [1 ]
Yang, Wenqing [1 ]
Hou, Shuaitao [1 ]
Xie, Dewen [2 ]
Yang, Jingxin [1 ]
Liu, Liwei [1 ]
Yang, Song [1 ]
机构
[1] Guizhou Univ, State Key Lab Breeding Base Green Pesticide & Agr, Key Lab Green Pesticide & Agr Bioengn, Minist Educ,Ctr R&D Fine Chem, Guiyang 550025, Peoples R China
[2] Guizhou Univ, Coll Pharm, Guiyang 550025, Peoples R China
基金
中国国家自然科学基金;
关键词
Antiviral activity; Atomic force microscopy; Transmission electron microscopy; Molecular docking; Virus disassembly;
D O I
10.1016/j.pestbp.2021.104771
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
A series of novel 1-phenyl-5-amine-4-pyrazole thioether derivatives containing a 1,3,4-oxadiazole moiety was designed and synthesised. In vivo antiviral bioassay results showed that most of the target compounds exhibited excellent inactivation activity against Tobacco mosaic virus (TMV). The EC50 values of the inactivation activities for T2, T7, T9, T24, T25 and T27 were 15.7, 15.7, 15.5, 11.9, 12.5 and 16.5 ?g/mL, respectively, which were remarkably superior over that of the commercialised antiviral agent ningnanmycin (40.3 ?g/mL). Morphological study using AFM and TEM of TMV treated with T24 showed that T24 could significantly shorten the polymerization length of TMV particles and formed a distinct break on the rod-shaped TMV. Investigations for virus infection efficiency on tobacco leaves demonstrated that infectivity of virion had been reduced obviously upon T24 treatment. Subsequently, a strong interaction between T24 and TMV-CP (Kd = 3.8 ?M, score 6.11) was observed through MST experiments. Molecular docking study further revealed that target compounds interact with amino acid residue Glu50 in TMV CP, causing disassembly of virion, shorting the length of the virion and reducing the infectivity of virion, and resulting in high inactivating activity of target compounds. This study provides a new insight for discovery of antiviral compounds through a new action mechanism with a new binding site.
引用
收藏
页数:9
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