AUTHOR=Kasho Kazutoshi , Oshima Taku , Chumsakul Onuma , Nakamura Kensuke , Fukamachi Kazuki , Katayama Tsutomu 

TITLE=Whole-Genome Analysis Reveals That the Nucleoid Protein IHF Predominantly Binds to the Replication Origin oriC Specifically at the Time of Initiation

JOURNAL=Frontiers in Microbiology

VOLUME=12

YEAR=2021

URL=https://www.frontiersin.org/journals/microbiology/articles/10.3389/fmicb.2021.697712

DOI=10.3389/fmicb.2021.697712

ISSN=1664-302X

ABSTRACT=<p>The structure and function of bacterial chromosomes are dynamically regulated by a wide variety of nucleoid-associated proteins (NAPs) and DNA superstructures, such as DNA supercoiling. In <italic>Escherichia coli</italic>, integration host factor (IHF), a NAP, binds to specific transcription promoters and regulatory DNA elements of DNA replication such as the replication origin <italic>oriC</italic>: binding to these elements depends on the cell cycle but underlying mechanisms are unknown. In this study, we combined GeF-seq (genome footprinting with high-throughput sequencing) with synchronization of the <italic>E. coli</italic> cell cycle to determine the genome-wide, cell cycle-dependent binding of IHF with base-pair resolution. The GeF-seq results in this study were qualified enough to analyze genomic IHF binding sites (e.g., <italic>oriC</italic> and the transcriptional promoters of <italic>ilvG</italic> and <italic>osmY</italic>) except some of the known sites. Unexpectedly, we found that before replication initiation, <italic>oriC</italic> was a predominant site for stable IHF binding, whereas all other loci exhibited reduced IHF binding. To reveal the specific mechanism of stable <italic>oriC–</italic>IHF binding, we inserted a truncated <italic>oriC</italic> sequence in the <italic>terC</italic> (replication terminus) locus of the genome. Before replication initiation, stable IHF binding was detected even at this additional <italic>oriC</italic> site, dependent on the specific DnaA-binding sequence DnaA box R1 within the site. DnaA oligomers formed on <italic>oriC</italic> might protect the <italic>oriC</italic>–IHF complex from IHF dissociation. After replication initiation, IHF rapidly dissociated from <italic>oriC</italic>, and IHF binding to other sites was sustained or stimulated. In addition, we identified a novel locus associated with cell cycle-dependent IHF binding. These findings provide mechanistic insight into IHF binding and dissociation in the genome.</p>