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nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids

The development of novel cancer therapeutic strategies has garnered increasing interest in cancer research. Among the therapeutic choices, chemosensitizers have shown exciting prospects. Peptides are an attractive alternative among the molecules that may be used as chemosensitizers. We rationally de...

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Autores principales: Trinidad-Calderón, Plinio Alejandro, López-Castillo, Laura Margarita, Gallegos-Martínez, Salvador, Trujillo-de Santiago, Grissel, García-Lara, Silverio, Álvarez, Mario Moisés
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9105272/
https://www.ncbi.nlm.nih.gov/pubmed/35566175
http://dx.doi.org/10.3390/molecules27092824
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author Trinidad-Calderón, Plinio Alejandro
López-Castillo, Laura Margarita
Gallegos-Martínez, Salvador
Trujillo-de Santiago, Grissel
García-Lara, Silverio
Álvarez, Mario Moisés
author_facet Trinidad-Calderón, Plinio Alejandro
López-Castillo, Laura Margarita
Gallegos-Martínez, Salvador
Trujillo-de Santiago, Grissel
García-Lara, Silverio
Álvarez, Mario Moisés
author_sort Trinidad-Calderón, Plinio Alejandro
collection PubMed
description The development of novel cancer therapeutic strategies has garnered increasing interest in cancer research. Among the therapeutic choices, chemosensitizers have shown exciting prospects. Peptides are an attractive alternative among the molecules that may be used as chemosensitizers. We rationally designed a new-to-nature peptide, nurP28, derived from the 22-kDa α-zein protein sequence (entry Q00919_MAIZE). The resultant sequence of the nurP28 peptide after the addition of arginine residues was LALLALLRLRRRATTAFIIP, and we added acetyl and amide groups at the N- and C-terminus, respectively, for capping. We evaluated the cytotoxicity of the nurP28 peptide alone and in combination with docetaxel in fibroblast monolayers and breast cancer monolayers and spheroids. Our results indicated that nurP28 is not cytotoxic to human fibroblasts or cancer cells. Nevertheless, when combined with 1 µM docetaxel, 3 ng/mL nurP28 induced equivalent (in MCF7 monolayers) and higher (in MCF7 spheroids) cytotoxic effects than 10-fold higher doses of docetaxel alone. These findings suggest that nurP28 may act as a chemosensitizer in breast cancer treatment. This study describes the enhancing “anti-cancer” effects of nurP28 in breast cancer 2D and 3D cultures treated with docetaxel. Further studies should explore the mechanisms underlying these effects and assess the clinical potential of our findings using animal models.
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spelling pubmed-91052722022-05-14 nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids Trinidad-Calderón, Plinio Alejandro López-Castillo, Laura Margarita Gallegos-Martínez, Salvador Trujillo-de Santiago, Grissel García-Lara, Silverio Álvarez, Mario Moisés Molecules Article The development of novel cancer therapeutic strategies has garnered increasing interest in cancer research. Among the therapeutic choices, chemosensitizers have shown exciting prospects. Peptides are an attractive alternative among the molecules that may be used as chemosensitizers. We rationally designed a new-to-nature peptide, nurP28, derived from the 22-kDa α-zein protein sequence (entry Q00919_MAIZE). The resultant sequence of the nurP28 peptide after the addition of arginine residues was LALLALLRLRRRATTAFIIP, and we added acetyl and amide groups at the N- and C-terminus, respectively, for capping. We evaluated the cytotoxicity of the nurP28 peptide alone and in combination with docetaxel in fibroblast monolayers and breast cancer monolayers and spheroids. Our results indicated that nurP28 is not cytotoxic to human fibroblasts or cancer cells. Nevertheless, when combined with 1 µM docetaxel, 3 ng/mL nurP28 induced equivalent (in MCF7 monolayers) and higher (in MCF7 spheroids) cytotoxic effects than 10-fold higher doses of docetaxel alone. These findings suggest that nurP28 may act as a chemosensitizer in breast cancer treatment. This study describes the enhancing “anti-cancer” effects of nurP28 in breast cancer 2D and 3D cultures treated with docetaxel. Further studies should explore the mechanisms underlying these effects and assess the clinical potential of our findings using animal models. MDPI 2022-04-29 /pmc/articles/PMC9105272/ /pubmed/35566175 http://dx.doi.org/10.3390/molecules27092824 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Trinidad-Calderón, Plinio Alejandro
López-Castillo, Laura Margarita
Gallegos-Martínez, Salvador
Trujillo-de Santiago, Grissel
García-Lara, Silverio
Álvarez, Mario Moisés
nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids
title nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids
title_full nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids
title_fullStr nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids
title_full_unstemmed nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids
title_short nurP28, a New-to-Nature Zein-Derived Peptide, Enhances the Therapeutic Effect of Docetaxel in Breast Cancer Monolayers and Spheroids
title_sort nurp28, a new-to-nature zein-derived peptide, enhances the therapeutic effect of docetaxel in breast cancer monolayers and spheroids
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9105272/
https://www.ncbi.nlm.nih.gov/pubmed/35566175
http://dx.doi.org/10.3390/molecules27092824
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