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Nucleosome DNA unwrapping does not affect prototype foamy virus integration efficiency or site selection.


ABSTRACT: Eukaryotic DNA binding proteins must access genomic DNA that is packaged into chromatin in vivo. During a productive infection, retroviral integrases (IN) must similarly interact with chromatin to integrate the viral cDNA genome. Here we examine the role of nucleosome DNA unwrapping in the retroviral integrase search for a target site. These studies utilized PFV intasomes that are comprised of a tetramer of PFV IN with two oligomers mimicking the viral cDNA ends. Modified recombinant human histones were used to generate nucleosomes with increased unwrapping rates at different DNA regions. These modifications included the acetylmimetic H3(K56Q) and the chemically engineered H4(K77ac, K79ac). While transcription factors and DNA damage sensors may search nucleosome bound DNA during transient unwrapping, PFV intasome mediated integration appears to be unaffected by increased nucleosome unwrapping. These studies suggest PFV intasomes do not utilize nucleosome unwrapping to search nucleosome targets.

SUBMITTER: Mackler RM 

PROVIDER: S-EPMC6415784 | biostudies-literature | 2019

REPOSITORIES: biostudies-literature

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Nucleosome DNA unwrapping does not affect prototype foamy virus integration efficiency or site selection.

Mackler Randi M RM   Jones Nathan D ND   Gardner Anne M AM   Lopez Miguel A MA   Howard Cecil J CJ   Fishel Richard R   Yoder Kristine E KE  

PloS one 20190313 3


Eukaryotic DNA binding proteins must access genomic DNA that is packaged into chromatin in vivo. During a productive infection, retroviral integrases (IN) must similarly interact with chromatin to integrate the viral cDNA genome. Here we examine the role of nucleosome DNA unwrapping in the retroviral integrase search for a target site. These studies utilized PFV intasomes that are comprised of a tetramer of PFV IN with two oligomers mimicking the viral cDNA ends. Modified recombinant human histo  ...[more]

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