Kinetic Pathways of Topology Simplification by Type-II Topoisomerases in Knotted Supercoiled DNA

Author:

Ziraldo Riccardo,Hanke Andreas,Levene Stephen D.

Abstract

ABSTRACTThe topological state of covalently closed, double-stranded DNA is defined by the knot type K and the linking-number difference ΔLk relative to unknotted relaxed DNA. DNA topoisomerases are essential enzymes that control the topology of DNA in all cells. In particular, type-II topoisomerases change both K and ΔLk by a duplex-strand-passage mechanism and have been shown to simplify the topology of DNA to levels below thermal equilibrium at the expense of ATP hydrolysis. It remains a puzzle how small enzymes are able to preferentially select strand passages that result in topology simplification in much larger DNA molecules. Using numerical simulations, we consider the non-equilibrium dynamics of transitions between topological states (K, ΔLk) in DNA induced by type-II topoisomerases. For a biological process that delivers DNA molecules in a given topological state (KLk) at a constant rate we fully characterize the pathways of topology simplification by type-II topoisomerases in terms of stationary probability distributions and probability currents on the network of topological states (KLk). In particular, we observe that type-II topoisomerase activity is significantly enhanced in DNA molecules that maintain a supercoiled state with constant torsional tension. This is relevant for bacterial cells in which torsional tension is maintained by enzyme-dependent homeostatic mechanisms such as DNA-gyrase activity.

Publisher

Cold Spring Harbor Laboratory

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