Molecular Determinants of Site-specific Inhibition of Human DNA Topoisomerase I by Fagaronine and Ethoxidine

Autor:	Igor Nabiev, Jean Claude Jardillier, Fabrice Fleury, Alain J.P. Alix, Anatoli Ianoul, Irina Kudelina, Jérôme Devy, Olivier Duval, Alyona Sukhanova
Rok vydání:	2000
Předmět:	biology Chemistry Stereochemistry Hydrogen bond Guanine Topoisomerase Cell Biology Cleavage (embryo) Biochemistry chemistry.chemical_compound DNA Intercalation Fagaronine biology.protein Molecular Biology Ternary complex DNA
Zdroj:	Journal of Biological Chemistry. 275:3501-3509
ISSN:	0021-9258
Popis:	DNA topoisomerase (top) I inhibition activity of the natural alkaloid fagaronine (NSC157995) and its new synthetic derivative ethoxidine (12-ethoxy-benzo[c]phenanthridine) has been correlated with their molecular interactions and sequence specificity within the DNA complexes. Flow linear dichroism shows that ethoxidine exhibits the same inhibition of DNA relaxation as fagaronine at the 10-fold lower concentration. The patterns of DNA cleavage by top I show linear enhancement of CPT-dependent sites at the 0.016–50 μm concentrations of fagaronine, whereas ethoxidine suppress both top I-specific and CPT-dependent sites. Suppression of top I-mediated cleavage by ethoxidine is found to be specific for the sites, including strand cut between A and T. Fagaronine and ethoxidine are DNA major groove intercalators. Ethoxidine intercalates DNA in A-T sequences and its 12-ethoxy-moiety (absent in fagaronine) extends into the DNA minor groove. These findings may explain specificity of suppression by ethoxidine of the strong top I cleavage sites with the A(+1), T(−1) immediately adjacent to the strand cut. Fagaronine does not show any sequence specificity of DNA intercalation, but its highly electronegative oxygen of hydroxy group (absent in ethoxidine) is shown to be an acceptor of the hydrogen bond with the NH2 group of G base of DNA. Ability of fagaronine to stabilize top I-mediated ternary complex is proposed to be determined by interaction of its hydroxy group with the guanine at position (+1) of the DNA cleavage site and of quaternary nitrogen interaction with top I. The model proposed provides a guidance for screening new top I-targeted drugs in terms of identification of molecular determinants responsible for their top I inhibition effects.
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=doi_________::cbb4c8411717df611664667ddf0abeb6 https://doi.org/10.1074/jbc.275.5.3501 Zobrazit plný text záznamu