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DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives

[Image: see text] A series of bis-N-substituted tetrandrine derivatives carrying different aromatic substituents attached to both nitrogen atoms of the natural alkaloid were studied with double-stranded model DNAs (dsDNAs) to examine the binding properties and mechanism. Variable-temperature molecul...

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Autores principales: González-Martínez, Sandra Mónica, Valencia-Ochoa, Drochss Pettry, Gálvez-Ruiz, Juan Carlos, Leyva-Peralta, Mario Alberto, Juárez-Sánchez, Octavio, Islas-Osuna, María A., Calvillo-Páez, Viviana Isabel, Höpfl, Herbert, Íñiguez-Palomares, Ramón, Rocha-Alonzo, Fernando, Ochoa Lara, Karen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2022
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9118212/
https://www.ncbi.nlm.nih.gov/pubmed/35601331
http://dx.doi.org/10.1021/acsomega.2c00225
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author González-Martínez, Sandra Mónica
Valencia-Ochoa, Drochss Pettry
Gálvez-Ruiz, Juan Carlos
Leyva-Peralta, Mario Alberto
Juárez-Sánchez, Octavio
Islas-Osuna, María A.
Calvillo-Páez, Viviana Isabel
Höpfl, Herbert
Íñiguez-Palomares, Ramón
Rocha-Alonzo, Fernando
Ochoa Lara, Karen
author_facet González-Martínez, Sandra Mónica
Valencia-Ochoa, Drochss Pettry
Gálvez-Ruiz, Juan Carlos
Leyva-Peralta, Mario Alberto
Juárez-Sánchez, Octavio
Islas-Osuna, María A.
Calvillo-Páez, Viviana Isabel
Höpfl, Herbert
Íñiguez-Palomares, Ramón
Rocha-Alonzo, Fernando
Ochoa Lara, Karen
author_sort González-Martínez, Sandra Mónica
collection PubMed
description [Image: see text] A series of bis-N-substituted tetrandrine derivatives carrying different aromatic substituents attached to both nitrogen atoms of the natural alkaloid were studied with double-stranded model DNAs (dsDNAs) to examine the binding properties and mechanism. Variable-temperature molecular recognition studies using UV–vis and fluorescence techniques revealed the thermodynamic parameters, ΔH, ΔS, and ΔG, showing that the tetrandrine derivatives exhibit high affinity toward dsDNA (K ≈ 10(5)–10(7) M(–1)), particularly the bis(methyl)anthraquinone (BAqT) and bis(ethyl)indole compounds (BInT). Viscometry experiments, ethidium displacement assays, and molecular modeling studies enabled elucidation of the possible binding mode, indicating that the compounds exhibit a synergic interaction mode involving intercalation of one of the N-aryl substituents and interaction of the molecular skeleton in the major groove of the dsDNA. Cytotoxicity tests of the derivatives with tumor and nontumor cell lines demonstrated low cytotoxicity of these compounds, with the exception of the bis(methyl)pyrene (BPyrT) derivative, which is significantly more cytotoxic than the remaining derivatives, with IC(50) values against the LS-180, A-549, and ARPE-19 cell lines that are similar to natural tetrandrine. Finally, complementary electrochemical characterization studies unveiled good electrochemical stability of the compounds.
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spelling pubmed-91182122022-05-20 DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives González-Martínez, Sandra Mónica Valencia-Ochoa, Drochss Pettry Gálvez-Ruiz, Juan Carlos Leyva-Peralta, Mario Alberto Juárez-Sánchez, Octavio Islas-Osuna, María A. Calvillo-Páez, Viviana Isabel Höpfl, Herbert Íñiguez-Palomares, Ramón Rocha-Alonzo, Fernando Ochoa Lara, Karen ACS Omega [Image: see text] A series of bis-N-substituted tetrandrine derivatives carrying different aromatic substituents attached to both nitrogen atoms of the natural alkaloid were studied with double-stranded model DNAs (dsDNAs) to examine the binding properties and mechanism. Variable-temperature molecular recognition studies using UV–vis and fluorescence techniques revealed the thermodynamic parameters, ΔH, ΔS, and ΔG, showing that the tetrandrine derivatives exhibit high affinity toward dsDNA (K ≈ 10(5)–10(7) M(–1)), particularly the bis(methyl)anthraquinone (BAqT) and bis(ethyl)indole compounds (BInT). Viscometry experiments, ethidium displacement assays, and molecular modeling studies enabled elucidation of the possible binding mode, indicating that the compounds exhibit a synergic interaction mode involving intercalation of one of the N-aryl substituents and interaction of the molecular skeleton in the major groove of the dsDNA. Cytotoxicity tests of the derivatives with tumor and nontumor cell lines demonstrated low cytotoxicity of these compounds, with the exception of the bis(methyl)pyrene (BPyrT) derivative, which is significantly more cytotoxic than the remaining derivatives, with IC(50) values against the LS-180, A-549, and ARPE-19 cell lines that are similar to natural tetrandrine. Finally, complementary electrochemical characterization studies unveiled good electrochemical stability of the compounds. American Chemical Society 2022-05-03 /pmc/articles/PMC9118212/ /pubmed/35601331 http://dx.doi.org/10.1021/acsomega.2c00225 Text en © 2022 The Authors. Published by American Chemical Society https://creativecommons.org/licenses/by-nc-nd/4.0/Permits non-commercial access and re-use, provided that author attribution and integrity are maintained; but does not permit creation of adaptations or other derivative works (https://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle González-Martínez, Sandra Mónica
Valencia-Ochoa, Drochss Pettry
Gálvez-Ruiz, Juan Carlos
Leyva-Peralta, Mario Alberto
Juárez-Sánchez, Octavio
Islas-Osuna, María A.
Calvillo-Páez, Viviana Isabel
Höpfl, Herbert
Íñiguez-Palomares, Ramón
Rocha-Alonzo, Fernando
Ochoa Lara, Karen
DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives
title DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives
title_full DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives
title_fullStr DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives
title_full_unstemmed DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives
title_short DNA-Binding Properties of Bis-N-substituted Tetrandrine Derivatives
title_sort dna-binding properties of bis-n-substituted tetrandrine derivatives
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9118212/
https://www.ncbi.nlm.nih.gov/pubmed/35601331
http://dx.doi.org/10.1021/acsomega.2c00225
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