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The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability

The murine leukaemia virus (MLV) gag gene encodes a small protein called p12 that is essential for the early steps of viral replication. The N- and C-terminal regions of p12 are sequentially acting domains, both required for p12 function. Defects in the C-terminal domain can be overcome by introduci...

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Autores principales: Wight, Darren J., Boucherit, Virginie C., Wanaguru, Madushi, Elis, Efrat, Hirst, Elizabeth M. A., Li, Wilson, Ehrlich, Marcelo, Bacharach, Eran, Bishop, Kate N.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4214797/
https://www.ncbi.nlm.nih.gov/pubmed/25356837
http://dx.doi.org/10.1371/journal.ppat.1004474
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author Wight, Darren J.
Boucherit, Virginie C.
Wanaguru, Madushi
Elis, Efrat
Hirst, Elizabeth M. A.
Li, Wilson
Ehrlich, Marcelo
Bacharach, Eran
Bishop, Kate N.
author_facet Wight, Darren J.
Boucherit, Virginie C.
Wanaguru, Madushi
Elis, Efrat
Hirst, Elizabeth M. A.
Li, Wilson
Ehrlich, Marcelo
Bacharach, Eran
Bishop, Kate N.
author_sort Wight, Darren J.
collection PubMed
description The murine leukaemia virus (MLV) gag gene encodes a small protein called p12 that is essential for the early steps of viral replication. The N- and C-terminal regions of p12 are sequentially acting domains, both required for p12 function. Defects in the C-terminal domain can be overcome by introducing a chromatin binding motif into the protein. However, the function of the N-terminal domain remains unknown. Here, we undertook a detailed analysis of the effects of p12 mutation on incoming viral cores. We found that both reverse transcription complexes and isolated mature cores from N-terminal p12 mutants have altered capsid complexes compared to wild type virions. Electron microscopy revealed that mature N-terminal p12 mutant cores have different morphologies, although immature cores appear normal. Moreover, in immunofluorescent studies, both p12 and capsid proteins were lost rapidly from N-terminal p12 mutant viral cores after entry into target cells. Importantly, we determined that p12 binds directly to the MLV capsid lattice. However, we could not detect binding of an N-terminally altered p12 to capsid. Altogether, our data imply that p12 stabilises the mature MLV core, preventing premature loss of capsid, and that this is mediated by direct binding of p12 to the capsid shell. In this manner, p12 is also retained in the pre-integration complex where it facilitates tethering to mitotic chromosomes. These data also explain our previous observations that modifications to the N-terminus of p12 alter the ability of particles to abrogate restriction by TRIM5alpha and Fv1, factors that recognise viral capsid lattices.
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spelling pubmed-42147972014-11-05 The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability Wight, Darren J. Boucherit, Virginie C. Wanaguru, Madushi Elis, Efrat Hirst, Elizabeth M. A. Li, Wilson Ehrlich, Marcelo Bacharach, Eran Bishop, Kate N. PLoS Pathog Research Article The murine leukaemia virus (MLV) gag gene encodes a small protein called p12 that is essential for the early steps of viral replication. The N- and C-terminal regions of p12 are sequentially acting domains, both required for p12 function. Defects in the C-terminal domain can be overcome by introducing a chromatin binding motif into the protein. However, the function of the N-terminal domain remains unknown. Here, we undertook a detailed analysis of the effects of p12 mutation on incoming viral cores. We found that both reverse transcription complexes and isolated mature cores from N-terminal p12 mutants have altered capsid complexes compared to wild type virions. Electron microscopy revealed that mature N-terminal p12 mutant cores have different morphologies, although immature cores appear normal. Moreover, in immunofluorescent studies, both p12 and capsid proteins were lost rapidly from N-terminal p12 mutant viral cores after entry into target cells. Importantly, we determined that p12 binds directly to the MLV capsid lattice. However, we could not detect binding of an N-terminally altered p12 to capsid. Altogether, our data imply that p12 stabilises the mature MLV core, preventing premature loss of capsid, and that this is mediated by direct binding of p12 to the capsid shell. In this manner, p12 is also retained in the pre-integration complex where it facilitates tethering to mitotic chromosomes. These data also explain our previous observations that modifications to the N-terminus of p12 alter the ability of particles to abrogate restriction by TRIM5alpha and Fv1, factors that recognise viral capsid lattices. Public Library of Science 2014-10-30 /pmc/articles/PMC4214797/ /pubmed/25356837 http://dx.doi.org/10.1371/journal.ppat.1004474 Text en © 2014 Wight 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
Wight, Darren J.
Boucherit, Virginie C.
Wanaguru, Madushi
Elis, Efrat
Hirst, Elizabeth M. A.
Li, Wilson
Ehrlich, Marcelo
Bacharach, Eran
Bishop, Kate N.
The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability
title The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability
title_full The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability
title_fullStr The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability
title_full_unstemmed The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability
title_short The N-Terminus of Murine Leukaemia Virus p12 Protein Is Required for Mature Core Stability
title_sort n-terminus of murine leukaemia virus p12 protein is required for mature core stability
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4214797/
https://www.ncbi.nlm.nih.gov/pubmed/25356837
http://dx.doi.org/10.1371/journal.ppat.1004474
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