Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.

Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.

Host base excision repair (BER) proteins that repair oxidative damage enhance HIV infection. These proteins include the oxidative DNA damage glycosylases 8-oxo-guanine DNA glycosylase (OGG1) and mutY homolog (MYH) as well as DNA polymerase beta (Polβ). While deletion of oxidative BER genes leads to...

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Main Authors: Geoffrey R Bennett, Ryan Peters, Xiao-hong Wang, Jeungphill Hanne, Robert W Sobol, Ralf Bundschuh, Richard Fishel, Kristine E Yoder
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4106905?pdf=render
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spelling doaj-356ae06ec6874e5ca4223e0fa58c37a72020-11-25T01:45:45ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0197e10316410.1371/journal.pone.0103164Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.Geoffrey R BennettRyan PetersXiao-hong WangJeungphill HanneRobert W SobolRalf BundschuhRichard FishelKristine E YoderHost base excision repair (BER) proteins that repair oxidative damage enhance HIV infection. These proteins include the oxidative DNA damage glycosylases 8-oxo-guanine DNA glycosylase (OGG1) and mutY homolog (MYH) as well as DNA polymerase beta (Polβ). While deletion of oxidative BER genes leads to decreased HIV infection and integration efficiency, the mechanism remains unknown. One hypothesis is that BER proteins repair the DNA gapped integration intermediate. An alternative hypothesis considers that the most common oxidative DNA base damages occur on guanines. The subtle consensus sequence preference at HIV integration sites includes multiple G:C base pairs surrounding the points of joining. These observations suggest a role for oxidative BER during integration targeting at the nucleotide level. We examined the hypothesis that BER repairs a gapped integration intermediate by measuring HIV infection efficiency in Polβ null cell lines complemented with active site point mutants of Polβ. A DNA synthesis defective mutant, but not a 5'dRP lyase mutant, rescued HIV infection efficiency to wild type levels; this suggested Polβ DNA synthesis activity is not necessary while 5'dRP lyase activity is required for efficient HIV infection. An alternate hypothesis that BER events in the host genome influence HIV integration site selection was examined by sequencing integration sites in OGG1 and MYH null cells. In the absence of these 8-oxo-guanine specific glycosylases the chromatin elements of HIV integration site selection remain the same as in wild type cells. However, the HIV integration site sequence preference at G:C base pairs is altered at several positions in OGG1 and MYH null cells. Inefficient HIV infection in the absence of oxidative BER proteins does not appear related to repair of the gapped integration intermediate; instead oxidative damage repair may participate in HIV integration site preference at the sequence level.http://europepmc.org/articles/PMC4106905?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Geoffrey R Bennett
Ryan Peters
Xiao-hong Wang
Jeungphill Hanne
Robert W Sobol
Ralf Bundschuh
Richard Fishel
Kristine E Yoder
spellingShingle Geoffrey R Bennett
Ryan Peters
Xiao-hong Wang
Jeungphill Hanne
Robert W Sobol
Ralf Bundschuh
Richard Fishel
Kristine E Yoder
Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.
PLoS ONE
author_facet Geoffrey R Bennett
Ryan Peters
Xiao-hong Wang
Jeungphill Hanne
Robert W Sobol
Ralf Bundschuh
Richard Fishel
Kristine E Yoder
author_sort Geoffrey R Bennett
title Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.
title_short Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.
title_full Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.
title_fullStr Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.
title_full_unstemmed Repair of oxidative DNA base damage in the host genome influences the HIV integration site sequence preference.
title_sort repair of oxidative dna base damage in the host genome influences the hiv integration site sequence preference.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Host base excision repair (BER) proteins that repair oxidative damage enhance HIV infection. These proteins include the oxidative DNA damage glycosylases 8-oxo-guanine DNA glycosylase (OGG1) and mutY homolog (MYH) as well as DNA polymerase beta (Polβ). While deletion of oxidative BER genes leads to decreased HIV infection and integration efficiency, the mechanism remains unknown. One hypothesis is that BER proteins repair the DNA gapped integration intermediate. An alternative hypothesis considers that the most common oxidative DNA base damages occur on guanines. The subtle consensus sequence preference at HIV integration sites includes multiple G:C base pairs surrounding the points of joining. These observations suggest a role for oxidative BER during integration targeting at the nucleotide level. We examined the hypothesis that BER repairs a gapped integration intermediate by measuring HIV infection efficiency in Polβ null cell lines complemented with active site point mutants of Polβ. A DNA synthesis defective mutant, but not a 5'dRP lyase mutant, rescued HIV infection efficiency to wild type levels; this suggested Polβ DNA synthesis activity is not necessary while 5'dRP lyase activity is required for efficient HIV infection. An alternate hypothesis that BER events in the host genome influence HIV integration site selection was examined by sequencing integration sites in OGG1 and MYH null cells. In the absence of these 8-oxo-guanine specific glycosylases the chromatin elements of HIV integration site selection remain the same as in wild type cells. However, the HIV integration site sequence preference at G:C base pairs is altered at several positions in OGG1 and MYH null cells. Inefficient HIV infection in the absence of oxidative BER proteins does not appear related to repair of the gapped integration intermediate; instead oxidative damage repair may participate in HIV integration site preference at the sequence level.
url http://europepmc.org/articles/PMC4106905?pdf=render
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