Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods

Background: Heat shock protein (Hsp90KDa) is a molecular chaperone involved in the process of cellular oncogenesis, hence its importance as a therapeutic target. Geldanamycin is an inhibitor of Hsp90 chaperone activity, which binds to the ATP binding site in the N-terminal domain of Hsp90. However,...

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Autores principales: Vivas-Reyes, Ricardo, Morales-Bayuelo, Alejando, Gueto, Carlos, Drosos, Juan C., Márquez Lázaro, Johana, Baldiris, Rosa, Ahumedo, Maicol, Vivas-Gomez, Catalina, Aparicio, Dilia
Formato: Online Artículo Texto
Lenguaje:English
Publicado: F1000 Research Limited 2020
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10521063/
https://www.ncbi.nlm.nih.gov/pubmed/37767457
http://dx.doi.org/10.12688/f1000research.20844.2
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author Vivas-Reyes, Ricardo
Morales-Bayuelo, Alejando
Gueto, Carlos
Drosos, Juan C.
Márquez Lázaro, Johana
Baldiris, Rosa
Ahumedo, Maicol
Vivas-Gomez, Catalina
Aparicio, Dilia
author_facet Vivas-Reyes, Ricardo
Morales-Bayuelo, Alejando
Gueto, Carlos
Drosos, Juan C.
Márquez Lázaro, Johana
Baldiris, Rosa
Ahumedo, Maicol
Vivas-Gomez, Catalina
Aparicio, Dilia
author_sort Vivas-Reyes, Ricardo
collection PubMed
description Background: Heat shock protein (Hsp90KDa) is a molecular chaperone involved in the process of cellular oncogenesis, hence its importance as a therapeutic target. Geldanamycin is an inhibitor of Hsp90 chaperone activity, which binds to the ATP binding site in the N-terminal domain of Hsp90. However, geldanamycin has shown hepatotoxic damage in clinical trials; for this reason, its use is not recommended. Taking advantage that geldanamycin binds successfully to Hsp90, many efforts have focused on the search for similar analogues, which have the same or better biological response and reduce the side effects of its predecessor; 17-AAG and 17-DMAG are examples of these analogues. Methods: In order to know the chemical factors influencing the growth or decay of the biological activity of geldanamycin analogues, different computational techniques such as docking, 3DQSAR and quantum similarity were used.  Moreover, the study quantified the interaction energy between amino acids residues of active side and geldanamycin analogues, through hybrid methodology (Autodock-PM6) and DFT indexes. Results: The evaluation of interaction energies showed that the interaction with Lys58 residue is essential for the union of the analogues to the active site of Hsp90, and improves its biological activity. This union is formed through a substituent on C-11 of the geldanamycin macrocycle. A small and attractor group was found as the main steric and electrostatic characteristic that substituents on C11 need in order to interact with Lys 58; behavior was observed with hydroxy and methoxy series of geldanamycin analogues, under study. Conclusion: This study contributes with new hybrid methodology (Autodock-PM6) for the generation of 3DQSAR models, which to consider the interactions between compounds and amino acids residues of Hsp90´s active site in the alignment generation. Additionally, quantum similarity and reactivity indices calculations using DFT were performed to know the non-covalent stabilization in the active site of these compounds.
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spelling pubmed-105210632023-09-27 Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods Vivas-Reyes, Ricardo Morales-Bayuelo, Alejando Gueto, Carlos Drosos, Juan C. Márquez Lázaro, Johana Baldiris, Rosa Ahumedo, Maicol Vivas-Gomez, Catalina Aparicio, Dilia F1000Res Research Article Background: Heat shock protein (Hsp90KDa) is a molecular chaperone involved in the process of cellular oncogenesis, hence its importance as a therapeutic target. Geldanamycin is an inhibitor of Hsp90 chaperone activity, which binds to the ATP binding site in the N-terminal domain of Hsp90. However, geldanamycin has shown hepatotoxic damage in clinical trials; for this reason, its use is not recommended. Taking advantage that geldanamycin binds successfully to Hsp90, many efforts have focused on the search for similar analogues, which have the same or better biological response and reduce the side effects of its predecessor; 17-AAG and 17-DMAG are examples of these analogues. Methods: In order to know the chemical factors influencing the growth or decay of the biological activity of geldanamycin analogues, different computational techniques such as docking, 3DQSAR and quantum similarity were used.  Moreover, the study quantified the interaction energy between amino acids residues of active side and geldanamycin analogues, through hybrid methodology (Autodock-PM6) and DFT indexes. Results: The evaluation of interaction energies showed that the interaction with Lys58 residue is essential for the union of the analogues to the active site of Hsp90, and improves its biological activity. This union is formed through a substituent on C-11 of the geldanamycin macrocycle. A small and attractor group was found as the main steric and electrostatic characteristic that substituents on C11 need in order to interact with Lys 58; behavior was observed with hydroxy and methoxy series of geldanamycin analogues, under study. Conclusion: This study contributes with new hybrid methodology (Autodock-PM6) for the generation of 3DQSAR models, which to consider the interactions between compounds and amino acids residues of Hsp90´s active site in the alignment generation. Additionally, quantum similarity and reactivity indices calculations using DFT were performed to know the non-covalent stabilization in the active site of these compounds. F1000 Research Limited 2020-04-16 /pmc/articles/PMC10521063/ /pubmed/37767457 http://dx.doi.org/10.12688/f1000research.20844.2 Text en Copyright: © 2020 Vivas-Reyes R et al. https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution Licence, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Vivas-Reyes, Ricardo
Morales-Bayuelo, Alejando
Gueto, Carlos
Drosos, Juan C.
Márquez Lázaro, Johana
Baldiris, Rosa
Ahumedo, Maicol
Vivas-Gomez, Catalina
Aparicio, Dilia
Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods
title Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods
title_full Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods
title_fullStr Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods
title_full_unstemmed Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods
title_short Study of interaction energies between residues of the active site of Hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods
title_sort study of interaction energies between residues of the active site of hsp90 and geldanamycin analogues using quantum mechanics/molecular mechanics methods
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10521063/
https://www.ncbi.nlm.nih.gov/pubmed/37767457
http://dx.doi.org/10.12688/f1000research.20844.2
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