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Inhibitors of Venezuelan Equine Encephalitis Virus Identified Based on Host Interaction Partners of Viral Non-Structural Protein 3

Viruses. 2021-08; 
Allison Bakovic, Nishank Bhalla, Farhang Alem, Catherine Campbell, Weidong Zhou, Aarthi Narayanan
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Mutagenesis Services … Mutation of the opal stop codon (UGA) in the TC-83 TaV-nLuc virus was performed by site-directed mutagenesis performed by GenScript to a strong, ochre stop codon (UAA) (Figure S1, in Supplementary Figure File). In vitro RNA transcription from plasmid DNA and virus … Get A Quote

摘要

Venezuelan equine encephalitis virus (VEEV) is a new world alphavirus and a category B select agent. Currently, no FDA-approved vaccines or therapeutics are available to treat VEEV exposure and resultant disease manifestations. The C-terminus of the VEEV non-structural protein 3 (nsP3) facilitates cell-specific and virus-specific host factor binding preferences among alphaviruses, thereby providing targets of interest when designing novel antiviral therapeutics. In this study, we utilized an overexpression construct encoding HA-tagged nsP3 to identify host proteins that interact with VEEV nsP3 by mass spectrometry. Bioinformatic analyses of the putative interactors identified 42 small molecules with the potenti... More

关键词

TFAP2A, Venezuelan equine encephalitis virus, eIF2S2, host-proteome, mass spectrometry, non-structural protein 3, small molecule inhibitors, viral proteome