DNA preference of indenoisoquinolines: a computational approach.

Org Biomol Chem

Bogazici University, Department of Chemistry, Bebek, 34342, Istanbul, Turkey.

Published: May 2023

AI Article Synopsis

  • Human topoisomerase IB (hTopoIB) is a protein that helps relax DNA supercoils by creating a nick in the DNA, and its inhibition can lead to cell death, making it a target for cancer treatments.
  • Camptothecin (CPT) and indenoisoquinoline (IQN) are two classes of compounds that inhibit hTopoIB by binding to nicked DNA, but they interact differently with DNA bases.
  • The study explored the binding affinities and mechanisms of CPT and an IQN derivative, aiming to inform the design of more effective cancer-fighting drugs that specifically target DNA interactions.

Article Abstract

The human topoisomerase IB (hTopoIB) enzyme is a monomeric protein that relaxes the supercoils on double-stranded DNA by forming a covalent DNA/hTopoIB complex by introducing a nick on the DNA strand. Inhibition of hTopoIB results in cell death, which makes this protein a strong target for the treatment of various cancer types, including small-cell lung cancers and ovarian cancers. Camptothecin (CPT) and indenoisoquinoline (IQN) classes of compounds inhibit the hTopoIB activity by intercalating to nicked DNA pairs; however, these inhibitors show different preferences towards DNA bases when bound to the DNA/hTopoIB complex. Here, we investigated the affinities of CPT and one IQN derivative towards different DNA base pairs. The two inhibitors showed different stacking behaviors in the intercalation site and interaction pattern with binding pocket residues, indicating that they have different inhibition mechanisms in the binding pocket that affects the base-pair selectivity. The results obtained from this study are expected to guide researchers in designing gene-specific and more potent compounds to fight cancer through hTopoIB poisoning.

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Source
http://dx.doi.org/10.1039/d3ob00162hDOI Listing

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