Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins

The coronavirus replicase-transcriptase complex is an assembly of viral and cellular proteins that mediate the synthesis of genome and subgenome-sized mRNAs in the virus-infected cell. Here, we report a genetic and functional analysis of 19 temperature-sensitive (ts) mutants of Murine hepatitis viru...

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Autores principales: Sawicki, Stanley G, Sawicki, Dorothea L, Younker, Diane, Meyer, Yvonne, Thiel, Volker, Stokes, Helen, Siddell, Stuart G
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2005
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1298938/
https://www.ncbi.nlm.nih.gov/pubmed/16341254
http://dx.doi.org/10.1371/journal.ppat.0010039
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author Sawicki, Stanley G
Sawicki, Dorothea L
Younker, Diane
Meyer, Yvonne
Thiel, Volker
Stokes, Helen
Siddell, Stuart G
author_facet Sawicki, Stanley G
Sawicki, Dorothea L
Younker, Diane
Meyer, Yvonne
Thiel, Volker
Stokes, Helen
Siddell, Stuart G
author_sort Sawicki, Stanley G
collection PubMed
description The coronavirus replicase-transcriptase complex is an assembly of viral and cellular proteins that mediate the synthesis of genome and subgenome-sized mRNAs in the virus-infected cell. Here, we report a genetic and functional analysis of 19 temperature-sensitive (ts) mutants of Murine hepatitis virus MHV-A59 that are unable to synthesize viral RNA when the infection is initiated and maintained at the non-permissive temperature. Both classical and biochemical complementation analysis leads us to predict that the majority of MHV-A59 ORF1a replicase gene products (non-structural proteins nsp1–nsp11) form a single complementation group (cistron1) while the replicase gene products encoded in ORF1b (non-structural proteins nsp12–nsp16) are able to function in trans and comprise at least three, and possibly five, further complementation groups (cistrons II–VI). Also, we have identified mutations in the non-structural proteins nsp 4, nsp5, nsp10, nsp12, nsp14, and nsp16 that are responsible for the ts phenotype of eight MHV-A59 mutants, which allows us to conclude that these proteins are essential for the assembly of a functional replicase-transcriptase complex. Finally, our analysis of viral RNA synthesis in ts mutant virus-infected cells allows us to discriminate three phenotypes with regard to the inability of specific mutants to synthesize viral RNA at the non-permissive temperature. Mutant LA ts6 appeared to be defective in continuing negative-strand synthesis, mutant Alb ts16 appeared to form negative strands but these were not utilized for positive-strand RNA synthesis, and mutant Alb ts22 was defective in the elongation of both positive- and negative-strand RNA. On the basis of these results, we propose a model that describes a pathway for viral RNA synthesis in MHV-A59-infected cells. Further biochemical analysis of these mutants should allow us to identify intermediates in this pathway and elucidate the precise function(s) of the viral replicase proteins involved.
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spelling pubmed-12989382005-12-09 Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins Sawicki, Stanley G Sawicki, Dorothea L Younker, Diane Meyer, Yvonne Thiel, Volker Stokes, Helen Siddell, Stuart G PLoS Pathog Research Article The coronavirus replicase-transcriptase complex is an assembly of viral and cellular proteins that mediate the synthesis of genome and subgenome-sized mRNAs in the virus-infected cell. Here, we report a genetic and functional analysis of 19 temperature-sensitive (ts) mutants of Murine hepatitis virus MHV-A59 that are unable to synthesize viral RNA when the infection is initiated and maintained at the non-permissive temperature. Both classical and biochemical complementation analysis leads us to predict that the majority of MHV-A59 ORF1a replicase gene products (non-structural proteins nsp1–nsp11) form a single complementation group (cistron1) while the replicase gene products encoded in ORF1b (non-structural proteins nsp12–nsp16) are able to function in trans and comprise at least three, and possibly five, further complementation groups (cistrons II–VI). Also, we have identified mutations in the non-structural proteins nsp 4, nsp5, nsp10, nsp12, nsp14, and nsp16 that are responsible for the ts phenotype of eight MHV-A59 mutants, which allows us to conclude that these proteins are essential for the assembly of a functional replicase-transcriptase complex. Finally, our analysis of viral RNA synthesis in ts mutant virus-infected cells allows us to discriminate three phenotypes with regard to the inability of specific mutants to synthesize viral RNA at the non-permissive temperature. Mutant LA ts6 appeared to be defective in continuing negative-strand synthesis, mutant Alb ts16 appeared to form negative strands but these were not utilized for positive-strand RNA synthesis, and mutant Alb ts22 was defective in the elongation of both positive- and negative-strand RNA. On the basis of these results, we propose a model that describes a pathway for viral RNA synthesis in MHV-A59-infected cells. Further biochemical analysis of these mutants should allow us to identify intermediates in this pathway and elucidate the precise function(s) of the viral replicase proteins involved. Public Library of Science 2005-12 2005-12-09 /pmc/articles/PMC1298938/ /pubmed/16341254 http://dx.doi.org/10.1371/journal.ppat.0010039 Text en Copyright: © 2005 Sawicki et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Sawicki, Stanley G
Sawicki, Dorothea L
Younker, Diane
Meyer, Yvonne
Thiel, Volker
Stokes, Helen
Siddell, Stuart G
Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins
title Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins
title_full Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins
title_fullStr Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins
title_full_unstemmed Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins
title_short Functional and Genetic Analysis of Coronavirus Replicase-Transcriptase Proteins
title_sort functional and genetic analysis of coronavirus replicase-transcriptase proteins
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1298938/
https://www.ncbi.nlm.nih.gov/pubmed/16341254
http://dx.doi.org/10.1371/journal.ppat.0010039
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