AI Article Synopsis

  • * Researchers used a crystal structure of these enzymes to create simulations of their functional states, focusing on the movements of DNA within their binding sites.
  • * The findings showed how different parts of the enzyme interact with DNA, enhancing our knowledge of their mechanisms and potential catalytic cycles.

Article Abstract

Type IIA DNA topoisomerases are complex molecular nanomachines that manage topological states of the DNA molecule in the cell and play a crucial role in cellular processes such as cell division and transcription. They are also established targets of cancer chemotherapy. Starting from the available crystal structure of a fully catalytic topoisomerase IIA homodimer from , we constructed three states of this molecular motor primarily changing the configurations of the DNA segment bound in the DNA gate and performed μs-long all-atom molecular simulations. A comprehensive analysis revealed a sliding motion within the DNA gate and a teamwork between the N-gate and DNA gate that may be associated with the necessary molecular events that allow passage of the T-segment of DNA. The observed movement of the ATPase dimer relative to the DNA domain was reflected in different interaction patterns between the K-loops of the transducer domain and the B-A-B form of the bound DNA. Based on the obtained results, we mapped simulated configurations to the structures in the proposed catalytic cycle through which type IIA topoisomerases exert their function and discussed the possible transition events. The results extend our understanding of the mechanism of action of type IIA topoisomerases and provide an atomistic interpretation of some of the observed features of these molecular motors.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10436251PMC
http://dx.doi.org/10.1016/j.csbj.2023.07.019DOI Listing

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