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Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway

The effect on the cytotoxicity against breast cancer cell lines of the substitution of (26)Met residue in the sequence of the Bovine Lactoferricin-derived dimeric peptide LfcinB (20-30)(2): ((20)RRWQWRMKKLG(30))(2)-K-Ahx with amino acids of different polarity was evaluated. The process of the synthe...

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Autores principales: Insuasty-Cepeda, Diego Sebastián, Barragán-Cárdenas, Andrea Carolina, Ochoa-Zarzosa, Alejandra, López-Meza, Joel E., Fierro-Medina, Ricardo, García-Castañeda, Javier Eduardo, Rivera-Monroy, Zuly Jenny
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7352952/
https://www.ncbi.nlm.nih.gov/pubmed/32604743
http://dx.doi.org/10.3390/ijms21124550
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author Insuasty-Cepeda, Diego Sebastián
Barragán-Cárdenas, Andrea Carolina
Ochoa-Zarzosa, Alejandra
López-Meza, Joel E.
Fierro-Medina, Ricardo
García-Castañeda, Javier Eduardo
Rivera-Monroy, Zuly Jenny
author_facet Insuasty-Cepeda, Diego Sebastián
Barragán-Cárdenas, Andrea Carolina
Ochoa-Zarzosa, Alejandra
López-Meza, Joel E.
Fierro-Medina, Ricardo
García-Castañeda, Javier Eduardo
Rivera-Monroy, Zuly Jenny
author_sort Insuasty-Cepeda, Diego Sebastián
collection PubMed
description The effect on the cytotoxicity against breast cancer cell lines of the substitution of (26)Met residue in the sequence of the Bovine Lactoferricin-derived dimeric peptide LfcinB (20-30)(2): ((20)RRWQWRMKKLG(30))(2)-K-Ahx with amino acids of different polarity was evaluated. The process of the synthesis of the LfcinB (20-30)(2) analog peptides was similar to the original peptide. The cytotoxic assays showed that some analog peptides exhibited a significant cytotoxic effect against breast cancer cell lines HTB-132 and MCF-7, suggesting that the substitution of the Met with amino acids of a hydrophobic nature drastically enhances its cytotoxicity against HTB-132 and MCF-7 cells, reaching IC(50) values up to 6 µM. In addition, these peptides have a selective effect, since they exhibit a lower cytotoxic effect on the non-tumorigenic cell line MCF-12. Interestingly, the cytotoxic effect is fast (90 min) and is maintained for up to 48 h. Additionally, through flow cytometry, it was found that the obtained dimeric peptides generate cell death through the apoptosis pathway and do not compromise the integrity of the cytoplasmic membrane, and there are intrinsic apoptotic events involved. These results show that the obtained peptides are extremely promising molecules for the future development of drugs for use against breast cancer.
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spelling pubmed-73529522020-07-15 Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway Insuasty-Cepeda, Diego Sebastián Barragán-Cárdenas, Andrea Carolina Ochoa-Zarzosa, Alejandra López-Meza, Joel E. Fierro-Medina, Ricardo García-Castañeda, Javier Eduardo Rivera-Monroy, Zuly Jenny Int J Mol Sci Article The effect on the cytotoxicity against breast cancer cell lines of the substitution of (26)Met residue in the sequence of the Bovine Lactoferricin-derived dimeric peptide LfcinB (20-30)(2): ((20)RRWQWRMKKLG(30))(2)-K-Ahx with amino acids of different polarity was evaluated. The process of the synthesis of the LfcinB (20-30)(2) analog peptides was similar to the original peptide. The cytotoxic assays showed that some analog peptides exhibited a significant cytotoxic effect against breast cancer cell lines HTB-132 and MCF-7, suggesting that the substitution of the Met with amino acids of a hydrophobic nature drastically enhances its cytotoxicity against HTB-132 and MCF-7 cells, reaching IC(50) values up to 6 µM. In addition, these peptides have a selective effect, since they exhibit a lower cytotoxic effect on the non-tumorigenic cell line MCF-12. Interestingly, the cytotoxic effect is fast (90 min) and is maintained for up to 48 h. Additionally, through flow cytometry, it was found that the obtained dimeric peptides generate cell death through the apoptosis pathway and do not compromise the integrity of the cytoplasmic membrane, and there are intrinsic apoptotic events involved. These results show that the obtained peptides are extremely promising molecules for the future development of drugs for use against breast cancer. MDPI 2020-06-26 /pmc/articles/PMC7352952/ /pubmed/32604743 http://dx.doi.org/10.3390/ijms21124550 Text en © 2020 by the authors. 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 (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Insuasty-Cepeda, Diego Sebastián
Barragán-Cárdenas, Andrea Carolina
Ochoa-Zarzosa, Alejandra
López-Meza, Joel E.
Fierro-Medina, Ricardo
García-Castañeda, Javier Eduardo
Rivera-Monroy, Zuly Jenny
Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway
title Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway
title_full Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway
title_fullStr Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway
title_full_unstemmed Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway
title_short Peptides Derived from (RRWQWRMKKLG)(2-)K-Ahx Induce Selective Cellular Death in Breast Cancer Cell Lines through Apoptotic Pathway
title_sort peptides derived from (rrwqwrmkklg)(2-)k-ahx induce selective cellular death in breast cancer cell lines through apoptotic pathway
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7352952/
https://www.ncbi.nlm.nih.gov/pubmed/32604743
http://dx.doi.org/10.3390/ijms21124550
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