Author: Sulea, Traian; Lindner, Holger A.; Purisima, Enrico O.; Ménard, Robert
Title: Binding siteâ€based classification of coronaviral papainâ€like proteases Cord-id: 0mr97rtq Document date: 2005_12_15
ID: 0mr97rtq
Snippet: The coronavirus replicase gene encodes one or two papainâ€like proteases (termed PL1pro and PL2pro) implicated in the Nâ€terminal processing of the replicase polyprotein and thus contributing to the formation of the viral replicase complex that mediates genome replication. Using consensus fold recognition with the 3Dâ€JURY metaâ€predictor followed by model building and refinement, we developed a structural model for the single PLpro present in the severe acute respiratory syndrome coronaviru
Document: The coronavirus replicase gene encodes one or two papainâ€like proteases (termed PL1pro and PL2pro) implicated in the Nâ€terminal processing of the replicase polyprotein and thus contributing to the formation of the viral replicase complex that mediates genome replication. Using consensus fold recognition with the 3Dâ€JURY metaâ€predictor followed by model building and refinement, we developed a structural model for the single PLpro present in the severe acute respiratory syndrome coronavirus (SCoV) genome, based on significant structural relationships to the catalytic core domain of HAUSP, a ubiquitinâ€specific protease (USP). By combining the SCoV PLpro model with comparative sequence analyses we show that all currently known coronaviral PLpros can be classified into two groups according to their binding site architectures. One group includes all PL2pros and some of the PL1pros, which are characterized by a restricted USPâ€like binding site. This group is designated the Râ€group. The remaining PL1pros from some of the coronaviruses form the other group, featuring a more open papainâ€like binding site, and is referred to as the Oâ€group. This twoâ€group, binding siteâ€based classification is consistent with experimental data accumulated to date for the specificity of PLproâ€mediated polyprotein processing and PLpro inhibition. It also provides an independent evaluation of the similarityâ€based annotation of PLproâ€mediated cleavage sites, as well as a basis for comparison with previous groupings based on phylogenetic analyses. Proteins 2006.
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