Barrier to autointegration factor (BAF) inhibits vaccinia virus intermediate transcription in the absence of the viral B1 kinase

Nouhou Ibrahim; April Wicklund; Augusta Jamin; Matthew S. Wiebe

doi:10.1016/j.virol.2013.07.002

Barrier to autointegration factor (BAF) inhibits vaccinia virus intermediate transcription in the absence of the viral B1 kinase

Nouhou Ibrahim, April Wicklund, Augusta Jamin, Matthew S. Wiebe

Veterinary and Biomedical Sciences

Research output: Contribution to journal › Article › peer-review

25 Scopus citations

Abstract

Barrier to autointegration factor (BAF/BANF1) is a cellular DNA-binding protein found in the nucleus and cytoplasm. Cytoplasmic BAF binds to foreign DNA and can act as a defense against vaccinia DNA replication. To evade BAF, vaccinia expresses the B1 kinase, which phosphorylates BAF and blocks its ability to bind DNA. Interestingly, B1 is also needed for viral intermediate gene expression via an unknown mechanism. Therefore, we evaluated the impact of B1-BAF signaling on vaccinia transcription. Strikingly, the decrease in vaccinia transcription caused by loss of B1 can be rescued by depletion of BAF. The repressive action of BAF is greatest on a viral promoter, and is more modest when non-vaccinia promoters are employed, which suggests BAF acts in a gene specific manner. These studies expand our understanding of the role of the B1 kinase during infection and provide the first evidence that BAF is a defense against viral gene expression.

Original language	English (US)
Pages (from-to)	363-373
Number of pages	11
Journal	Virology
Volume	444
Issue number	1-2
DOIs	https://doi.org/10.1016/j.virol.2013.07.002
State	Published - Sep 2013

Keywords

BAF
BANF1
Barrier to autointegration
Transcription
Vaccinia
Virus host interaction

ASJC Scopus subject areas

Virology

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10.1016/j.virol.2013.07.002

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title = "Barrier to autointegration factor (BAF) inhibits vaccinia virus intermediate transcription in the absence of the viral B1 kinase",

abstract = "Barrier to autointegration factor (BAF/BANF1) is a cellular DNA-binding protein found in the nucleus and cytoplasm. Cytoplasmic BAF binds to foreign DNA and can act as a defense against vaccinia DNA replication. To evade BAF, vaccinia expresses the B1 kinase, which phosphorylates BAF and blocks its ability to bind DNA. Interestingly, B1 is also needed for viral intermediate gene expression via an unknown mechanism. Therefore, we evaluated the impact of B1-BAF signaling on vaccinia transcription. Strikingly, the decrease in vaccinia transcription caused by loss of B1 can be rescued by depletion of BAF. The repressive action of BAF is greatest on a viral promoter, and is more modest when non-vaccinia promoters are employed, which suggests BAF acts in a gene specific manner. These studies expand our understanding of the role of the B1 kinase during infection and provide the first evidence that BAF is a defense against viral gene expression.",

keywords = "BAF, BANF1, Barrier to autointegration, Transcription, Vaccinia, Virus host interaction",

author = "Nouhou Ibrahim and April Wicklund and Augusta Jamin and Wiebe, {Matthew S.}",

note = "Funding Information: This research was supported through NIH grants to M.W. ( 1K22 AI080941 , 1R56 AI099062 ) and the Nebraska Center for Virology ( 1P20 RR15635 ). N.I. and A.J. were partially supported by a Ruth L. Kirschstein NRSA ( 1T32 AIO60547 ). We also thank Drs. Paula Traktman and Kathy Boyle at the Medical College of Wisconsin for editorial suggestions and helpful scientific discussions. ",

year = "2013",

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doi = "10.1016/j.virol.2013.07.002",

language = "English (US)",

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journal = "Virology",

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AU - Wicklund, April

AU - Jamin, Augusta

AU - Wiebe, Matthew S.

N1 - Funding Information: This research was supported through NIH grants to M.W. ( 1K22 AI080941 , 1R56 AI099062 ) and the Nebraska Center for Virology ( 1P20 RR15635 ). N.I. and A.J. were partially supported by a Ruth L. Kirschstein NRSA ( 1T32 AIO60547 ). We also thank Drs. Paula Traktman and Kathy Boyle at the Medical College of Wisconsin for editorial suggestions and helpful scientific discussions.

PY - 2013/9

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N2 - Barrier to autointegration factor (BAF/BANF1) is a cellular DNA-binding protein found in the nucleus and cytoplasm. Cytoplasmic BAF binds to foreign DNA and can act as a defense against vaccinia DNA replication. To evade BAF, vaccinia expresses the B1 kinase, which phosphorylates BAF and blocks its ability to bind DNA. Interestingly, B1 is also needed for viral intermediate gene expression via an unknown mechanism. Therefore, we evaluated the impact of B1-BAF signaling on vaccinia transcription. Strikingly, the decrease in vaccinia transcription caused by loss of B1 can be rescued by depletion of BAF. The repressive action of BAF is greatest on a viral promoter, and is more modest when non-vaccinia promoters are employed, which suggests BAF acts in a gene specific manner. These studies expand our understanding of the role of the B1 kinase during infection and provide the first evidence that BAF is a defense against viral gene expression.

AB - Barrier to autointegration factor (BAF/BANF1) is a cellular DNA-binding protein found in the nucleus and cytoplasm. Cytoplasmic BAF binds to foreign DNA and can act as a defense against vaccinia DNA replication. To evade BAF, vaccinia expresses the B1 kinase, which phosphorylates BAF and blocks its ability to bind DNA. Interestingly, B1 is also needed for viral intermediate gene expression via an unknown mechanism. Therefore, we evaluated the impact of B1-BAF signaling on vaccinia transcription. Strikingly, the decrease in vaccinia transcription caused by loss of B1 can be rescued by depletion of BAF. The repressive action of BAF is greatest on a viral promoter, and is more modest when non-vaccinia promoters are employed, which suggests BAF acts in a gene specific manner. These studies expand our understanding of the role of the B1 kinase during infection and provide the first evidence that BAF is a defense against viral gene expression.

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Barrier to autointegration factor (BAF) inhibits vaccinia virus intermediate transcription in the absence of the viral B1 kinase

Abstract

Keywords

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