4x2y Citations

Structure determination of Murine Norovirus NS6 proteases with C-terminal extensions designed to probe protease-substrate interactions.

OpenAccess logo PeerJ 3 e798 (2015)
Related entries: 4ash, 4x2v, 4x2w, 4x2x

Cited: 9 times
EuropePMC logo PMID: 25755927

Abstract

Noroviruses are positive-sense single-stranded RNA viruses. They encode an NS6 protease that cleaves a viral polyprotein at specific sites to produce mature viral proteins. In an earlier study we obtained crystals of murine norovirus (MNV) NS6 protease in which crystal contacts were mediated by specific insertion of the C-terminus of one protein (which contains residues P5-P1 of the NS6-7 cleavage junction) into the peptide binding site of an adjacent molecule, forming an adventitious protease-product complex. We sought to reproduce this crystal form to investigate protease-substrate complexes by extending the C-terminus of NS6 construct to include residues on the C-terminal (P') side of the cleavage junction. We report the crystallization and crystal structure determination of inactive mutants of murine norovirus NS6 protease with C-terminal extensions of one, two and four residues from the N-terminus of the adjacent NS7 protein (NS6 1', NS6 2', NS6 4'). We also determined the structure of a chimeric extended NS6 protease in which the P4-P4' sequence of the NS6-7 cleavage site was replaced with the corresponding sequence from the NS2-3 cleavage junction (NS6 4' 2|3).The constructs NS6 1' and NS6 2' yielded crystals that diffracted anisotropically. We found that, although the uncorrected data could be phased by molecular replacement, refinement of the structures stalled unless the data were ellipsoidally truncated and corrected with anisotropic B-factors. These corrections significantly improved phasing by molecular replacement and subsequent refinement.The refined structures of all four extended NS6 proteases are very similar in structure to the mature MNV NS6-and in one case reveal additional details of a surface loop. Although the packing arrangement observed showed some similarities to those observed in the adventitious protease-product crystals reported previously, in no case were specific protease-substrate interactions observed.

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Reviews citing this publication (2)

  1. Norovirus Infection: Replication, Manipulation of Host, and Interaction with the Host Immune Response. Sarvestani ST, Cotton B, Fritzlar S, O'Donnell TB, Mackenzie JM. J Interferon Cytokine Res 36 215-225 (2016)
  2. Current tools for norovirus drug discovery. Weerasekara S, Prior AM, Hua DH. Expert Opin Drug Discov 11 529-541 (2016)

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  1. Viral and metazoan poxins are cGAMP-specific nucleases that restrict cGAS-STING signalling. Eaglesham JB, Pan Y, Kupper TS, Kranzusch PJ. Nature 566 259-263 (2019)
  2. Mouse Norovirus Infection Arrests Host Cell Translation Uncoupled from the Stress Granule-PKR-eIF2α Axis. Fritzlar S, Aktepe TE, Chao YW, Kenney ND, McAllaster MR, Wilen CB, White PA, Mackenzie JM. mBio 10 e00960-19 (2019)
  3. A Cell-based Fluorescence Resonance Energy Transfer (FRET) Sensor Reveals Inter- and Intragenogroup Variations in Norovirus Protease Activity and Polyprotein Cleavage. Emmott E, Sweeney TR, Goodfellow I. J Biol Chem 290 27841-27853 (2015)
  4. A Proposal for a Structural Model of the Feline Calicivirus Protease Bound to the Substrate Peptide under Physiological Conditions. Yokoyama M, Oka T, Takagi H, Kojima H, Okabe T, Nagano T, Tohya Y, Sato H. Front Microbiol 8 1383 (2017)
  5. In crystallo-screening for discovery of human norovirus 3C-like protease inhibitors. Guo J, Douangamath A, Song W, Coker AR, Chan AWE, Wood SP, Cooper JB, Resnick E, London N, Delft FV. J Struct Biol X 4 100031 (2020)
  6. Crystal Structure of Inhibitor-Bound GII.4 Sydney 2012 Norovirus 3C-Like Protease. Eruera AR, McSweeney AM, McKenzie-Goldsmith GM, Opel-Reading HK, Thomas SX, Campbell AC, Stubbing L, Siow A, Hubert JG, Brimble MA, Ward VK, Krause KL. Viruses 15 2202 (2023)


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