Literature DB >> 9391109

Yeast mutations in multiple complementation groups inhibit brome mosaic virus RNA replication and transcription and perturb regulated expression of the viral polymerase-like gene.

M Ishikawa1, J Díez, M Restrepo-Hartwig, P Ahlquist.   

Abstract

Brome mosaic virus (BMV), a member of the alphavirus-like superfamily of positive-strand RNA viruses, encodes two proteins, 1a and 2a, that interact with each other, with unidentified host proteins, and with host membranes to form the viral RNA replication complex. Yeast expressing 1a and 2a support replication and subgenomic mRNA synthesis by BMV RNA3 derivatives. Using a multistep selection and screening process, we have isolated yeast mutants in multiple complementation groups that inhibit BMV-directed gene expression. Three complementation groups, represented by mutants mab1-1, mab2-1, and mab3-1 (for maintenance of BMV functions), were selected for initial study. Each of these mutants has a single, recessive, chromosomal mutation that inhibits accumulation of positive- and negative-strand RNA3 and subgenomic mRNA. BMV-directed gene expression was inhibited when the RNA replication template was introduced by in vivo transcription from DNA or by transfection of yeast with in vitro transcripts, confirming that cytoplasmic RNA replication steps were defective. mab1-1, mab2-1, and mab3-1 slowed yeast growth to varying degrees and were temperature-sensitive, showing that the affected genes contribute to normal cell growth. In wild-type yeast, expression of the helicase-like 1a protein increased the accumulation of 2a mRNA and the polymerase-like 2a protein, revealing a new level of viral regulation. In association with their other effects, mab1-1 and mab2-1 blocked the ability of 1a to stimulate 2a mRNA and protein accumulation, whereas mab3-1 had elevated 2a protein accumulation. Together, these results show that BMV RNA replication in yeast depends on multiple host genes, some of which directly or indirectly affect the regulated expression and accumulation of 2a.

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Year:  1997        PMID: 9391109      PMCID: PMC28389          DOI: 10.1073/pnas.94.25.13810

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  26 in total

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Authors:  U K Schmitz; D M Lonsdale; R A Jefferson
Journal:  Curr Genet       Date:  1990-03       Impact factor: 3.886

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Authors:  S Froshauer; J Kartenbeck; A Helenius
Journal:  J Cell Biol       Date:  1988-12       Impact factor: 10.539

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  37 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  2001-02-20       Impact factor: 11.205

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4.  Alternate, virus-induced membrane rearrangements support positive-strand RNA virus genome replication.

Authors:  Michael Schwartz; Jianbo Chen; Wai-Ming Lee; Michael Janda; Paul Ahlquist
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5.  Efficient in vitro system of homologous recombination in brome mosaic bromovirus.

Authors:  Rafal Wierzchoslawski; Jozef J Bujarski
Journal:  J Virol       Date:  2006-06       Impact factor: 5.103

6.  Selectable viruses and altered susceptibility mutants in Arabidopsis thaliana.

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Journal:  Proc Natl Acad Sci U S A       Date:  1999-01-19       Impact factor: 11.205

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Authors:  J A den Boon; J Chen; P Ahlquist
Journal:  J Virol       Date:  2001-12       Impact factor: 5.103

8.  Brome mosaic virus RNA replication protein 1a dramatically increases in vivo stability but not translation of viral genomic RNA3.

Authors:  M Janda; P Ahlquist
Journal:  Proc Natl Acad Sci U S A       Date:  1998-03-03       Impact factor: 11.205

9.  The cellular decapping activators LSm1, Pat1, and Dhh1 control the ratio of subgenomic to genomic Flock House virus RNAs.

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