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Structure of the Vesicular Stomatitis Virus L Protein in Complex with Its Phosphoprotein Cofactor

Simon Jenni, Louis-Marie Bloyet, Rubén Díaz-Avalos, Bo Liang, Sean P. J. Whelan, Nikolaus Grigorieff, Stephen C. Harrison

2020Cell Reports85 citationsDOIOpen Access PDF

Abstract

The large (L) proteins of non-segmented, negative-strand RNA viruses are multifunctional enzymes that produce capped, methylated, and polyadenylated mRNA and replicate the viral genome. A phosphoprotein (P), required for efficient RNA-dependent RNA polymerization from the viral ribonucleoprotein (RNP) template, regulates the function and conformation of the L protein. We report the structure of vesicular stomatitis virus L in complex with its P cofactor determined by electron cryomicroscopy at 3.0 Å resolution, enabling us to visualize bound segments of P. The contacts of three P segments with multiple L domains show how P induces a closed, compact, initiation-competent conformation. Binding of P to L positions its N-terminal domain adjacent to a putative RNA exit channel for efficient encapsidation of newly synthesized genomes with the nucleoprotein and orients its C-terminal domain to interact with an RNP template. The model shows that a conserved tryptophan in the priming loop can support the initiating 5' nucleotide.

Topics & Concepts

PhosphoproteinVesicular stomatitis virusRNABiologyNucleoproteinRibonucleoproteinViral proteinPolyadenylationCell biologyMolecular biologyVirusVirologyBiochemistryPhosphorylationGeneVirology and Viral DiseasesAnimal Virus Infections StudiesViral Infections and Vectors