Rational design of 2 H-chromene-based antiphytovirals that inhibit virion assembly by outcompeting virus capsid-RNA interactions

Xiong Yang; Deguo Liu; Chunle Wei; Jianzhuan Li; Chunni Zhao; Yanping Tian; Xiangdong Li; Baoan Song; Runjiang Song

doi:10.1016/j.isci.2024.111210

Rational design of 2 H-chromene-based antiphytovirals that inhibit virion assembly by outcompeting virus capsid-RNA interactions

iScience. 2024 Oct 18;27(11):111210. doi: 10.1016/j.isci.2024.111210. eCollection 2024 Nov 15.

Authors

Xiong Yang¹, Deguo Liu², Chunle Wei¹, Jianzhuan Li¹, Chunni Zhao¹, Yanping Tian², Xiangdong Li², Baoan Song¹, Runjiang Song¹

Affiliations

¹ National Key Laboratory of Green Pesticide, Key Laboratory of Green Pesticide and Agricultural Bioengineering, Ministry of Education, Center for R & D of Fine Chemicals of Guizhou University, Guiyang City, Guizhou Province 550025, P.R. China.
² College of Plant Protection, Shandong Agricultural University, Tai'an City, Shandong Province 271018, P.R. China.

Abstract

Although the determination of the structural basis of potato virus Y (PVY) coat protein (CP) provides the possibility for CP-based antiviral drug design, the role of many specific residues on CP in regulating virion pathogenicity is largely unknown, and fewer small-molecular drugs have been discovered to act on these potential sites. In this study, a series of derivatives of 2,2-dimethyl-2H-chromene are rationally designed by employing a molecular hybridization strategy. We screen a case of phytovirucide C50 that could form a stable H-bond with Ser¹²⁵ of PVY CP to exert antiviral properties. Ser¹²⁵ is further identified to be crucial for CP-viral RNA (vRNA) interaction, enabling PVY virion assembly. This interaction can be significantly inhibited through competitive binding with compound C50. The study enhances our understanding of anti-PVY drug mechanisms and provides a basis for developing new CP-targeting virus particle assembly inhibitors.

Keywords: Biochemistry; Chemistry; Virology.