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Bacterial histone HBb from Bdellovibrio bacteriovorus compacts DNA by bending.

Yimin HuSamuel SchwabSilvia DeissPedro EscudeiroThor van HeeschJoe D JoinerJocelyne VreedeMarcus D HartmannAndrei N LupasBirte Hernandez AlvarezVikram AlvaRemus Thei Dame
Published in: Nucleic acids research (2024)
Histones are essential for genome compaction and transcription regulation in eukaryotes, where they assemble into octamers to form the nucleosome core. In contrast, archaeal histones assemble into dimers that form hypernucleosomes upon DNA binding. Although histone homologs have been identified in bacteria recently, their DNA-binding characteristics remain largely unexplored. Our study reveals that the bacterial histone HBb (Bd0055) is indispensable for the survival of Bdellovibrio bacteriovorus, suggesting critical roles in DNA organization and gene regulation. By determining crystal structures of free and DNA-bound HBb, we unveil its distinctive dimeric assembly, diverging from those of eukaryotic and archaeal histones, while also elucidating how it binds and bends DNA through interaction interfaces reminiscent of eukaryotic and archaeal histones. Building on this, by employing various biophysical and biochemical approaches, we further substantiated the ability of HBb to bind and compact DNA by bending in a sequence-independent manner. Finally, using DNA affinity purification and sequencing, we reveal that HBb binds along the entire genomic DNA of B. bacteriovorus without sequence specificity. These distinct DNA-binding properties of bacterial histones, showcasing remarkable similarities yet significant differences from their archaeal and eukaryotic counterparts, highlight the diverse roles histones play in DNA organization across all domains of life.
Keyphrases
  • dna binding
  • circulating tumor
  • cell free
  • single molecule
  • transcription factor
  • dna methylation
  • nucleic acid
  • magnetic resonance
  • gene expression
  • circulating tumor cells
  • magnetic resonance imaging
  • single cell
  • low cost