Author: Ye, Qiaozhen; West, Alan M.V.; Silletti, Steve; Corbett, Kevin D.
Title: Architecture and selfâ€assembly of the SARSâ€CoVâ€2 nucleocapsid protein Cord-id: 0nioym64 Document date: 2020_7_12
ID: 0nioym64
Snippet: The COVIDâ€2019 pandemic is the most severe acute public health threat of the twentyâ€first century. To properly address this crisis with both robust testing and novel treatments, we require a deep understanding of the life cycle of the causative agent, the SARSâ€CoVâ€2 coronavirus. Here, we examine the architecture and selfâ€assembly properties of the SARSâ€CoVâ€2 nucleocapsid protein, which packages viral RNA into new virions. We determined a 1.4 Ã¥ resolution crystal structure of this
Document: The COVIDâ€2019 pandemic is the most severe acute public health threat of the twentyâ€first century. To properly address this crisis with both robust testing and novel treatments, we require a deep understanding of the life cycle of the causative agent, the SARSâ€CoVâ€2 coronavirus. Here, we examine the architecture and selfâ€assembly properties of the SARSâ€CoVâ€2 nucleocapsid protein, which packages viral RNA into new virions. We determined a 1.4 Ã¥ resolution crystal structure of this protein's N2b domain, revealing a compact, intertwined dimer similar to that of related coronaviruses including SARSâ€CoV. While the N2b domain forms a dimer in solution, addition of the Câ€terminal spacer B/N3 domain mediates formation of a homotetramer. Using hydrogenâ€deuterium exchange mass spectrometry, we find evidence that at least part of this putatively disordered domain is structured, potentially forming an αâ€helix that selfâ€associates and cooperates with the N2b domain to mediate tetramer formation. Finally, we map the locations of amino acid substitutions in the N protein from over 38,000 SARSâ€CoVâ€2 genome sequences. We find that these substitutions are strongly clustered in the protein's N2a linker domain, and that substitutions within the N1b and N2b domains cluster away from their functional RNA binding and dimerization interfaces. Overall, this work reveals the architecture and selfâ€assembly properties of a key protein in the SARSâ€CoVâ€2 life cycle, with implications for both drug design and antibodyâ€based testing. This article is protected by copyright. All rights reserved.
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