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The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60

Amphibian secretions have been extensively investigated for the production of bioactive molecules. Salamandrin-I is an antioxidant peptide, isolated from the skin secretion of the fire salamander, that has induced no toxicity in microglia or erythrocytes. Importantly, the administration of antioxida...

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Autores principales: Silva-Carvalho, Amandda Évelin, de Oliveira, Nakaly Natiely, Machado, Julia Viana Lafetá, Moreira, Daniel Carneiro, Brand, Guilherme Dotto, Leite, José Roberto S. A., Plácido, Alexandra, Eaton, Peter, Saldanha-Araujo, Felipe
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10384876/
https://www.ncbi.nlm.nih.gov/pubmed/37514049
http://dx.doi.org/10.3390/pharmaceutics15071864
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author Silva-Carvalho, Amandda Évelin
de Oliveira, Nakaly Natiely
Machado, Julia Viana Lafetá
Moreira, Daniel Carneiro
Brand, Guilherme Dotto
Leite, José Roberto S. A.
Plácido, Alexandra
Eaton, Peter
Saldanha-Araujo, Felipe
author_facet Silva-Carvalho, Amandda Évelin
de Oliveira, Nakaly Natiely
Machado, Julia Viana Lafetá
Moreira, Daniel Carneiro
Brand, Guilherme Dotto
Leite, José Roberto S. A.
Plácido, Alexandra
Eaton, Peter
Saldanha-Araujo, Felipe
author_sort Silva-Carvalho, Amandda Évelin
collection PubMed
description Amphibian secretions have been extensively investigated for the production of bioactive molecules. Salamandrin-I is an antioxidant peptide, isolated from the skin secretion of the fire salamander, that has induced no toxicity in microglia or erythrocytes. Importantly, the administration of antioxidants may constitute an adequate therapeutic approach to cancer treatment. Here, with the purpose of better characterizing the therapeutic potential of salamandrin-I, we investigated whether this antioxidant peptide also exerts anticancer activity, using the human leukemia cell line HL-60 as a cancer model. Salamandrin-I treatment induced a significant reduction in HL-60 proliferation, which was accompanied by cell cycle arrest. Furthermore, the peptide-induced cell death showed a significant increase in the LDH release in HL-60 cells. The cellular toxicity exerted by salamandrin-I is possibly related to pyroptosis, since the HL-60 cells showed loss of mitochondrial membrane potential and hyperexpression of inflammasome components following the peptide treatment. This is the first demonstration of the anticancer potential of the salamandrin-I peptide. Such results are important, as they offer relevant insights into the field of cancer therapy and allow the design of future bioactive molecules using salamandrin-I as a template.
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spelling pubmed-103848762023-07-30 The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60 Silva-Carvalho, Amandda Évelin de Oliveira, Nakaly Natiely Machado, Julia Viana Lafetá Moreira, Daniel Carneiro Brand, Guilherme Dotto Leite, José Roberto S. A. Plácido, Alexandra Eaton, Peter Saldanha-Araujo, Felipe Pharmaceutics Article Amphibian secretions have been extensively investigated for the production of bioactive molecules. Salamandrin-I is an antioxidant peptide, isolated from the skin secretion of the fire salamander, that has induced no toxicity in microglia or erythrocytes. Importantly, the administration of antioxidants may constitute an adequate therapeutic approach to cancer treatment. Here, with the purpose of better characterizing the therapeutic potential of salamandrin-I, we investigated whether this antioxidant peptide also exerts anticancer activity, using the human leukemia cell line HL-60 as a cancer model. Salamandrin-I treatment induced a significant reduction in HL-60 proliferation, which was accompanied by cell cycle arrest. Furthermore, the peptide-induced cell death showed a significant increase in the LDH release in HL-60 cells. The cellular toxicity exerted by salamandrin-I is possibly related to pyroptosis, since the HL-60 cells showed loss of mitochondrial membrane potential and hyperexpression of inflammasome components following the peptide treatment. This is the first demonstration of the anticancer potential of the salamandrin-I peptide. Such results are important, as they offer relevant insights into the field of cancer therapy and allow the design of future bioactive molecules using salamandrin-I as a template. MDPI 2023-07-01 /pmc/articles/PMC10384876/ /pubmed/37514049 http://dx.doi.org/10.3390/pharmaceutics15071864 Text en © 2023 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
Silva-Carvalho, Amandda Évelin
de Oliveira, Nakaly Natiely
Machado, Julia Viana Lafetá
Moreira, Daniel Carneiro
Brand, Guilherme Dotto
Leite, José Roberto S. A.
Plácido, Alexandra
Eaton, Peter
Saldanha-Araujo, Felipe
The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60
title The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60
title_full The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60
title_fullStr The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60
title_full_unstemmed The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60
title_short The Peptide Salamandrin-I Modulates Components Involved in Pyroptosis and Induces Cell Death in Human Leukemia Cell Line HL-60
title_sort peptide salamandrin-i modulates components involved in pyroptosis and induces cell death in human leukemia cell line hl-60
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10384876/
https://www.ncbi.nlm.nih.gov/pubmed/37514049
http://dx.doi.org/10.3390/pharmaceutics15071864
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