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Tobacco Necrosis Virus-A(C) Single Coat Protein Amino Acid Substitutions Determine Host-Specific Systemic Infections Of Nicotiana Benthamiana And Soybean

MOLECULAR PLANT-MICROBE INTERACTIONS(2021)

Cited 9|Views31
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Abstract
Plant viruses often infect several distinct host species. Sometimes, viruses can systemically infect a specific host whereas, in other cases, only local infections occur in other species. How viral and host factors interact to determine systemic infections among different hosts is largely unknown, particularly for icosahedral positive-stranded RNA viruses. The Tobacco necrosis virus-A Chinese isolate belongs to the genus Alphanecro virus in the family Tombusviridae. In this study, we investigated variations in systemic infections of tobacco necrosis virus-A(C) (TNV-A(C)) in Nicotiana benthamiana and Glycine max (soybean) by alanine-scanning mutagenesis of the viral coat protein (CP), which is essential for systemic movement of TNV-A(C). We found that three amino acids, R-169, K-177, and Q(233), are key residues that mediate varying degrees of systemic infections of N. benthamiana and soybean. Further analysis revealed that variations in systemic trafficking of TNV-A(C) CP mutants in N. benthamiana and soybean are associated with virion assembly and stability. The CP amino acids K-177 and Q(233) are highly conserved among all TNV-A isolates and are replaced by Q and K in the TNV-D isolates. We demonstrated that systemic infectivity of either TNV-A(C) K177A and Q233A or K177Q and Q233K mutants are correlated with the binding affinity of the mutated CPs to the host-specific Hsc70-2 protein. These results expand our understanding of host-dependent long-distance movement of icosahedral viruses in plants.
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Key words
coat protein, Hsc70-2, host-dependent systemic infection, site-directed mutagenesis, tobacco necrosis virus-A, virion assembly, virion stability
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