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Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.

According to the present model for assembly of alphaviruses, e.g. Semliki Forest virus (SFV), the viral genome is first encapsidated into a nucleocapsid (NC) in cytoplasm and this is then used for budding at plasma membrane (PM). The preformed NC is thought to act as a template on which the viral en...

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Detalles Bibliográficos
Autores principales: Forsell, K, Griffiths, G, Garoff, H
Formato: Texto
Lenguaje:English
Publicado: 1996
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC452474/
https://www.ncbi.nlm.nih.gov/pubmed/8978676
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author Forsell, K
Griffiths, G
Garoff, H
author_facet Forsell, K
Griffiths, G
Garoff, H
author_sort Forsell, K
collection PubMed
description According to the present model for assembly of alphaviruses, e.g. Semliki Forest virus (SFV), the viral genome is first encapsidated into a nucleocapsid (NC) in cytoplasm and this is then used for budding at plasma membrane (PM). The preformed NC is thought to act as a template on which the viral envelope can be organized. In the present work we have characterized two SFV deletion mutants which did not assemble NCs in the cytoplasm but which instead appeared to form NCs at the PM simultaneously with virus budding. The deletions were introduced in a conserved 14 residue long linker peptide that joins the amino-terminal RNA-binding domain with the carboxy-terminal serine-protease domain of the capsid protein. Despite the deletions and the change in morphogenesis, wild-type (wt)-like particles were produced with almost wt efficiency. It is suggested that the NC assembly defect of the mutants is rescued through spike-capsid interactions at PM. The results show that the preassembly of NCs in the cytoplasm is not a prerequisite for alphavirus budding. The apparent similarities of the morphogenesis pathways of wt and mutant SFV with those of type D and type C retroviruses are discussed.
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spelling pubmed-4524742005-04-27 Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding. Forsell, K Griffiths, G Garoff, H EMBO J Research Article According to the present model for assembly of alphaviruses, e.g. Semliki Forest virus (SFV), the viral genome is first encapsidated into a nucleocapsid (NC) in cytoplasm and this is then used for budding at plasma membrane (PM). The preformed NC is thought to act as a template on which the viral envelope can be organized. In the present work we have characterized two SFV deletion mutants which did not assemble NCs in the cytoplasm but which instead appeared to form NCs at the PM simultaneously with virus budding. The deletions were introduced in a conserved 14 residue long linker peptide that joins the amino-terminal RNA-binding domain with the carboxy-terminal serine-protease domain of the capsid protein. Despite the deletions and the change in morphogenesis, wild-type (wt)-like particles were produced with almost wt efficiency. It is suggested that the NC assembly defect of the mutants is rescued through spike-capsid interactions at PM. The results show that the preassembly of NCs in the cytoplasm is not a prerequisite for alphavirus budding. The apparent similarities of the morphogenesis pathways of wt and mutant SFV with those of type D and type C retroviruses are discussed. 1996-12-02 /pmc/articles/PMC452474/ /pubmed/8978676 Text en
spellingShingle Research Article
Forsell, K
Griffiths, G
Garoff, H
Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.
title Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.
title_full Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.
title_fullStr Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.
title_full_unstemmed Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.
title_short Preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.
title_sort preformed cytoplasmic nucleocapsids are not necessary for alphavirus budding.
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC452474/
https://www.ncbi.nlm.nih.gov/pubmed/8978676
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