Dynamic and facilitated binding of topoisomerase accelerates topological relaxation

Author:

Michieletto Davide12ORCID,Fosado Yair A G1,Melas Elias1,Baiesi Marco34,Tubiana Luca567,Orlandini Enzo34

Affiliation:

1. School of Physics and Astronomy, University of Edinburgh, Peter Guthrie Tait Road, Edinburgh EH9 3FD, UK

2. MRC Human Genetics Unit, Institute of Genetics and Cancer, University of Edinburgh, Edinburgh EH4 2XU, UK

3. Department of Physics and Astronomy, University of Padova, Via Marzolo 8, I-35131 Padova, Italy

4. INFN, Sezione di Padova, Via Marzolo 8, I-35131 Padova, Italy

5. Physics Department, University of Trento, via Sommarive 14, I-38123 Trento, Italy

6. INFN-TIFPA, Trento Institute for Fundamental Physics and Applications, I-38123 Trento, Italy

7. Faculty of Physics, University of Vienna, Boltzmanngasse 5, 1090 Vienna, Austria

Abstract

Abstract How type 2 Topoisomerase (TopoII) proteins relax and simplify the topology of DNA molecules is one of the most intriguing open questions in genome and DNA biophysics. Most of the existing models neglect the dynamics of TopoII which is expected of proteins searching their targets via facilitated diffusion. Here, we show that dynamic binding of TopoII speeds up the topological relaxation of knotted substrates by enhancing the search of the knotted arc. Intriguingly, this in turn implies that the timescale of topological relaxation is virtually independent of the substrate length. We then discover that considering binding biases due to facilitated diffusion on looped substrates steers the sampling of the topological space closer to the boundaries between different topoisomers yielding an optimally fast topological relaxation. We discuss our findings in the context of topological simplification in vitro and in vivo.

Funder

European Research Council

Royal Society

MIUR

Publisher

Oxford University Press (OUP)

Subject

Genetics

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