Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain

The key enzyme in coronavirus polyprotein processing is the viral main proteinase, M(pro), a protein with extremely low sequence similarity to other viral and cellular proteinases. Here, the crystal structure of the 33.1 kDa transmissible gastroenteritis (corona)virus M(pro) is reported. The structu...

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Autores principales: Anand, Kanchan, Palm, Gottfried J., Mesters, Jeroen R., Siddell, Stuart G., Ziebuhr, John, Hilgenfeld, Rolf
Formato: Texto
Lenguaje:English
Publicado: Oxford University Press 2002
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC126080/
https://www.ncbi.nlm.nih.gov/pubmed/12093723
http://dx.doi.org/10.1093/emboj/cdf327
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author Anand, Kanchan
Palm, Gottfried J.
Mesters, Jeroen R.
Siddell, Stuart G.
Ziebuhr, John
Hilgenfeld, Rolf
author_facet Anand, Kanchan
Palm, Gottfried J.
Mesters, Jeroen R.
Siddell, Stuart G.
Ziebuhr, John
Hilgenfeld, Rolf
author_sort Anand, Kanchan
collection PubMed
description The key enzyme in coronavirus polyprotein processing is the viral main proteinase, M(pro), a protein with extremely low sequence similarity to other viral and cellular proteinases. Here, the crystal structure of the 33.1 kDa transmissible gastroenteritis (corona)virus M(pro) is reported. The structure was refined to 1.96 Å resolution and revealed three dimers in the asymmetric unit. The mutual arrangement of the protomers in each of the dimers suggests that M(pro) self-processing occurs in trans. The active site, comprised of Cys144 and His41, is part of a chymotrypsin-like fold that is connected by a 16 residue loop to an extra domain featuring a novel α-helical fold. Molecular modelling and mutagenesis data implicate the loop in substrate binding and elucidate S1 and S2 subsites suitable to accommodate the side chains of the P1 glutamine and P2 leucine residues of M(pro) substrates. Interactions involving the N-terminus and the α-helical domain stabilize the loop in the orientation required for trans-cleavage activity. The study illustrates that RNA viruses have evolved unprecedented variations of the classical chymotrypsin fold.
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spelling pubmed-1260802002-09-19 Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain Anand, Kanchan Palm, Gottfried J. Mesters, Jeroen R. Siddell, Stuart G. Ziebuhr, John Hilgenfeld, Rolf EMBO J Article The key enzyme in coronavirus polyprotein processing is the viral main proteinase, M(pro), a protein with extremely low sequence similarity to other viral and cellular proteinases. Here, the crystal structure of the 33.1 kDa transmissible gastroenteritis (corona)virus M(pro) is reported. The structure was refined to 1.96 Å resolution and revealed three dimers in the asymmetric unit. The mutual arrangement of the protomers in each of the dimers suggests that M(pro) self-processing occurs in trans. The active site, comprised of Cys144 and His41, is part of a chymotrypsin-like fold that is connected by a 16 residue loop to an extra domain featuring a novel α-helical fold. Molecular modelling and mutagenesis data implicate the loop in substrate binding and elucidate S1 and S2 subsites suitable to accommodate the side chains of the P1 glutamine and P2 leucine residues of M(pro) substrates. Interactions involving the N-terminus and the α-helical domain stabilize the loop in the orientation required for trans-cleavage activity. The study illustrates that RNA viruses have evolved unprecedented variations of the classical chymotrypsin fold. Oxford University Press 2002-07-01 /pmc/articles/PMC126080/ /pubmed/12093723 http://dx.doi.org/10.1093/emboj/cdf327 Text en Copyright © 2002 European Molecular Biology Organization
spellingShingle Article
Anand, Kanchan
Palm, Gottfried J.
Mesters, Jeroen R.
Siddell, Stuart G.
Ziebuhr, John
Hilgenfeld, Rolf
Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain
title Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain
title_full Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain
title_fullStr Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain
title_full_unstemmed Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain
title_short Structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain
title_sort structure of coronavirus main proteinase reveals combination of a chymotrypsin fold with an extra α-helical domain
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC126080/
https://www.ncbi.nlm.nih.gov/pubmed/12093723
http://dx.doi.org/10.1093/emboj/cdf327
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