Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors

BACKGROUND AND PURPOSE: Colorectal and prostate cancers are two of the most common types and cause of a high rate of deaths worldwide. Therefore, any strategy to stop or at least slacken the development and progression of malignant cells is an important therapeutic choice. The aim of the present wor...

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Autores principales: Zanni, Riccardo, Galvez-Llompart, Maria, Morell, Cecilia, Rodríguez-Henche, Nieves, Díaz-Laviada, Inés, Recio-Iglesias, Maria Carmen, Garcia-Domenech, Ramon, Galvez, Jorge
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4409212/
https://www.ncbi.nlm.nih.gov/pubmed/25910265
http://dx.doi.org/10.1371/journal.pone.0124244
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author Zanni, Riccardo
Galvez-Llompart, Maria
Morell, Cecilia
Rodríguez-Henche, Nieves
Díaz-Laviada, Inés
Recio-Iglesias, Maria Carmen
Garcia-Domenech, Ramon
Galvez, Jorge
author_facet Zanni, Riccardo
Galvez-Llompart, Maria
Morell, Cecilia
Rodríguez-Henche, Nieves
Díaz-Laviada, Inés
Recio-Iglesias, Maria Carmen
Garcia-Domenech, Ramon
Galvez, Jorge
author_sort Zanni, Riccardo
collection PubMed
description BACKGROUND AND PURPOSE: Colorectal and prostate cancers are two of the most common types and cause of a high rate of deaths worldwide. Therefore, any strategy to stop or at least slacken the development and progression of malignant cells is an important therapeutic choice. The aim of the present work is the identification of novel cancer chemotherapy agents. Nowadays, many different drug discovery approaches are available, but this paper focuses on Molecular Topology, which has already demonstrated its extraordinary efficacy in this field, particularly in the identification of new hit and lead compounds against cancer. This methodology uses the graph theoretical formalism to numerically characterize molecular structures through the so called topological indices. Once obtained a specific framework, it allows the construction of complex mathematical models that can be used to predict physical, chemical or biological properties of compounds. In addition, Molecular Topology is highly efficient in selecting and designing new hit and lead drugs. According to the aforementioned, Molecular Topology has been applied here for the construction of specific Akt/mTOR and β-catenin inhibition mathematical models in order to identify and select novel antitumor agents. EXPERIMENTAL APPROACH: Based on the results obtained by the selected mathematical models, six novel potential inhibitors of the Akt/mTOR and β-catenin pathways were identified. These compounds were then tested in vitro to confirm their biological activity. CONCLUSION AND IMPLICATIONS: Five of the selected compounds, CAS n° 256378-54-8 (Inhibitor n°1), 663203-38-1 (Inhibitor n°2), 247079-73-8 (Inhibitor n°3), 689769-86-6 (Inhibitor n°4) and 431925-096 (Inhibitor n°6) gave positive responses and resulted to be active for Akt/mTOR and/or β-catenin inhibition. This study confirms once again the Molecular Topology’s reliability and efficacy to find out novel drugs in the field of cancer.
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spelling pubmed-44092122015-05-12 Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors Zanni, Riccardo Galvez-Llompart, Maria Morell, Cecilia Rodríguez-Henche, Nieves Díaz-Laviada, Inés Recio-Iglesias, Maria Carmen Garcia-Domenech, Ramon Galvez, Jorge PLoS One Research Article BACKGROUND AND PURPOSE: Colorectal and prostate cancers are two of the most common types and cause of a high rate of deaths worldwide. Therefore, any strategy to stop or at least slacken the development and progression of malignant cells is an important therapeutic choice. The aim of the present work is the identification of novel cancer chemotherapy agents. Nowadays, many different drug discovery approaches are available, but this paper focuses on Molecular Topology, which has already demonstrated its extraordinary efficacy in this field, particularly in the identification of new hit and lead compounds against cancer. This methodology uses the graph theoretical formalism to numerically characterize molecular structures through the so called topological indices. Once obtained a specific framework, it allows the construction of complex mathematical models that can be used to predict physical, chemical or biological properties of compounds. In addition, Molecular Topology is highly efficient in selecting and designing new hit and lead drugs. According to the aforementioned, Molecular Topology has been applied here for the construction of specific Akt/mTOR and β-catenin inhibition mathematical models in order to identify and select novel antitumor agents. EXPERIMENTAL APPROACH: Based on the results obtained by the selected mathematical models, six novel potential inhibitors of the Akt/mTOR and β-catenin pathways were identified. These compounds were then tested in vitro to confirm their biological activity. CONCLUSION AND IMPLICATIONS: Five of the selected compounds, CAS n° 256378-54-8 (Inhibitor n°1), 663203-38-1 (Inhibitor n°2), 247079-73-8 (Inhibitor n°3), 689769-86-6 (Inhibitor n°4) and 431925-096 (Inhibitor n°6) gave positive responses and resulted to be active for Akt/mTOR and/or β-catenin inhibition. This study confirms once again the Molecular Topology’s reliability and efficacy to find out novel drugs in the field of cancer. Public Library of Science 2015-04-24 /pmc/articles/PMC4409212/ /pubmed/25910265 http://dx.doi.org/10.1371/journal.pone.0124244 Text en © 2015 Zanni et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Zanni, Riccardo
Galvez-Llompart, Maria
Morell, Cecilia
Rodríguez-Henche, Nieves
Díaz-Laviada, Inés
Recio-Iglesias, Maria Carmen
Garcia-Domenech, Ramon
Galvez, Jorge
Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors
title Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors
title_full Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors
title_fullStr Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors
title_full_unstemmed Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors
title_short Novel Cancer Chemotherapy Hits by Molecular Topology: Dual Akt and Beta-Catenin Inhibitors
title_sort novel cancer chemotherapy hits by molecular topology: dual akt and beta-catenin inhibitors
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4409212/
https://www.ncbi.nlm.nih.gov/pubmed/25910265
http://dx.doi.org/10.1371/journal.pone.0124244
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