Alpha 2.0
Login Register
» Articles » PMID: 9748568

DNA Sequence Selectivity of Topoisomerases and Topoisomerase Poisons

Overview
Journal Biochim Biophys Acta
Specialties Biochemistry
Biophysics
Date 1998 Sep 28
PMID 9748568
Citations 40
Authors
G Capranico
M Binaschi
Affiliations
Soon will be listed here.
Abstract

Chemical agents able to interfere with DNA topoisomerases are widespread in nature, and some of them have clinical efficacy as antitumor or antibacterial drugs. Drugs which have as a target DNA topoisomerases could be divided into two categories: poisons and catalytic inhibitors. Classical topoisomerase poisons stimulate cleavage in a sequence-selective manner, yielding drug-specific cleavage intensity pattern. The mechanisms of drug interaction with DNA topoisomerases, the DNA sequence selectivity of the action of topoisomerase II poisons and the identification of structural determinants of their activity have suggested that topoisomerase II poisons may fit into a specific pharmacophore, constituted by a planar ring system with DNA intercalation or intercalation-like properties, and protruding side chains interfering with the protein side of the covalent enzyme-DNA complex. The complete definition of the diverse pharmacophores of topoisomerase II poisons will certainly be of value for the design of new agents directed to specific genomic sites, and more effective in the treatment of human cancer.

Citing Articles

Highly sensitive mapping of in vitro type II topoisomerase DNA cleavage sites with SHAN-seq.

Morgan I, McKie S, Kim R, Seol Y, Xu J, Harami G Nucleic Acids Res. 2024; 52(16):9777-9787.

PMID: 39106172 PMC: 11381365. DOI: 10.1093/nar/gkae638.

Highly sensitive mapping of type II topoisomerase DNA cleavage sites with SHAN-seq.

Morgan I, McKie S, Kim R, Seol Y, Xu J, Harami G bioRxiv. 2024; .

PMID: 38798569 PMC: 11118536. DOI: 10.1101/2024.05.17.594727.

Evaluation of the Anticancer and Biological Activities of Istaroxime via Ex Vivo Analyses, Molecular Docking and Conceptual Density Functional Theory Computations.

Gok E, Unal N, Gungor B, Karakus G, Kaya S, Canturk P Molecules. 2023; 28(22).

PMID: 38005181 PMC: 10672917. DOI: 10.3390/molecules28227458.

DNA topoisomerase inhibition with the HIF inhibitor acriflavine promotes transcription of lncRNAs in endothelial cells.

Seredinski S, Boos F, Gunther S, Oo J, Warwick T, Izquierdo Ponce J Mol Ther Nucleic Acids. 2022; 27:1023-1035.

PMID: 35228897 PMC: 8844413. DOI: 10.1016/j.omtn.2022.01.016.

Debulking of topoisomerase DNA-protein crosslinks (TOP-DPC) by the proteasome, non-proteasomal and non-proteolytic pathways.

Sun Y, Saha L, Saha S, Jo U, Pommier Y DNA Repair (Amst). 2020; 94:102926.

PMID: 32674013 PMC: 9210512. DOI: 10.1016/j.dnarep.2020.102926.