Disentangling DNA molecules

Phys Life Rev. 2016 Sep:18:118-134. doi: 10.1016/j.plrev.2016.05.001. Epub 2016 May 4.

Abstract

The widespread circular form of DNA molecules inside cells creates very serious topological problems during replication. Due to the helical structure of the double helix the parental strands of circular DNA form a link of very high order, and yet they have to be unlinked before the cell division. DNA topoisomerases, the enzymes that catalyze passing of one DNA segment through another, solve this problem in principle. However, it is very difficult to remove all entanglements between the replicated DNA molecules due to huge length of DNA comparing to the cell size. One strategy that nature uses to overcome this problem is to create the topoisomerases that can dramatically reduce the fraction of linked circular DNA molecules relative to the corresponding fraction at thermodynamic equilibrium. This striking property of the enzymes means that the enzymes that interact with DNA only locally can access their topology, a global property of circular DNA molecules. This review considers the experimental studies of the phenomenon and analyzes the theoretical models that have been suggested in attempts to explain it. We describe here how various models of enzyme action can be investigated computationally. There is no doubt at the moment that we understand basic principles governing enzyme action. Still, there are essential quantitative discrepancies between the experimental data and the theoretical predictions. We consider how these discrepancies can be overcome.

Keywords: DNA; DNA topoisomerases; DNA topology; Topology simplification.

Publication types

  • Review

MeSH terms

  • DNA Topoisomerases, Type II
  • DNA* / chemistry
  • DNA* / metabolism
  • Models, Molecular

Substances

  • DNA
  • DNA Topoisomerases, Type II