Integration host factor bends and bridges DNA in a multiplicity of binding modes with varying specificity

Author:

Yoshua Samuel B1,Watson George D1ORCID,Howard Jamieson A L1,Velasco-Berrelleza Victor1,Leake Mark C12ORCID,Noy Agnes1ORCID

Affiliation:

1. Department of Physics, University of York, York YO10 5DD, UK

2. Department of Biology, University of York, York YO10 5DD, UK

Abstract

Abstract Nucleoid-associated proteins (NAPs) are crucial in organizing prokaryotic DNA and regulating genes. Vital to these activities are complex nucleoprotein structures, however, how these form remains unclear. Integration host factor (IHF) is an Escherichia coli NAP that creates very sharp bends in DNA at sequences relevant to several functions including transcription and recombination, and is also responsible for general DNA compaction when bound non-specifically. We show that IHF–DNA structural multimodality is more elaborate than previously thought, and provide insights into how this drives mechanical switching towards strongly bent DNA. Using single-molecule atomic force microscopy and atomic molecular dynamics simulations we find three binding modes in roughly equal proportions: ‘associated’ (73° of DNA bend), ‘half-wrapped’ (107°) and ‘fully-wrapped’ (147°), only the latter occurring with sequence specificity. We show IHF bridges two DNA double helices through non-specific recognition that gives IHF a stoichiometry greater than one and enables DNA mesh assembly. We observe that IHF-DNA structural multiplicity is driven through non-specific electrostatic interactions that we anticipate to be a general NAP feature for physical organization of chromosomes.

Funder

Engineering and Physical Sciences Research Council

Biology and Biotechnology Research Council

Leverhulme Trust

CONACYT

Publisher

Oxford University Press (OUP)

Subject

Genetics

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