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Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens

Among the strategies employed to overcome the development of multidrug-resistant bacteria, directed chemotherapy combined with local therapies (e.g., magnetic hyperthermia) has gained great interest. A nano-assembly coupling the antimicrobial peptide AS-48 to biomimetic magnetic nanoparticles (AS-48...

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Autores principales: Gaglio, Salvatore Calogero, Jabalera, Ylenia, Montalbán-López, Manuel, Millán-Placer, Ana Cristina, Lázaro-Callejón, Marina, Maqueda, Mercedes, Carrasco-Jimenez, María Paz, Laso, Alejandro, Aínsa, José A., Iglesias, Guillermo R., Perduca, Massimiliano, López, Concepción Jiménez
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9785849/
https://www.ncbi.nlm.nih.gov/pubmed/36559238
http://dx.doi.org/10.3390/pharmaceutics14122744
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author Gaglio, Salvatore Calogero
Jabalera, Ylenia
Montalbán-López, Manuel
Millán-Placer, Ana Cristina
Lázaro-Callejón, Marina
Maqueda, Mercedes
Carrasco-Jimenez, María Paz
Laso, Alejandro
Aínsa, José A.
Iglesias, Guillermo R.
Perduca, Massimiliano
López, Concepción Jiménez
author_facet Gaglio, Salvatore Calogero
Jabalera, Ylenia
Montalbán-López, Manuel
Millán-Placer, Ana Cristina
Lázaro-Callejón, Marina
Maqueda, Mercedes
Carrasco-Jimenez, María Paz
Laso, Alejandro
Aínsa, José A.
Iglesias, Guillermo R.
Perduca, Massimiliano
López, Concepción Jiménez
author_sort Gaglio, Salvatore Calogero
collection PubMed
description Among the strategies employed to overcome the development of multidrug-resistant bacteria, directed chemotherapy combined with local therapies (e.g., magnetic hyperthermia) has gained great interest. A nano-assembly coupling the antimicrobial peptide AS-48 to biomimetic magnetic nanoparticles (AS-48-BMNPs) was demonstrated to have potent bactericidal effects on both Gram-positive and Gram-negative bacteria when the antimicrobial activity of the peptide was combined with magnetic hyperthermia. Nevertheless, intracellular pathogens remain challenging due to the difficulty of the drug reaching the bacterium. Thus, improving the cellular uptake of the nanocarrier is crucial for the success of the treatment. In the present study, we demonstrate the embedding cellular uptake of the original nano-assembly into THP-1, reducing the toxicity of AS-48 toward healthy THP-1 cells. We optimized the design of PLGA[AS-48-BMNPs] in terms of size, colloidal stability, and hyperthermia activity (either magnetic or photothermal). The stability of the nano-formulation at physiological pH values was evaluated by studying the AS-48 release at this pH value. The influence of pH and hyperthermia on the AS-48 release from the nano-formulation was also studied. These results show a slower AS-48 release from PLGA[AS-48-BMNPs] compared to previous nano-formulations, which could make this new nano-formulation suitable for longer extended treatments of intracellular pathogens. PLGA[AS-48-BMNPs] are internalized in THP-1 cells where AS-48 is liberated slowly, which may be useful to treat diseases and prevent infection caused by intracellular pathogens. The treatment will be more efficient combined with hyperthermia or photothermia.
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spelling pubmed-97858492022-12-24 Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens Gaglio, Salvatore Calogero Jabalera, Ylenia Montalbán-López, Manuel Millán-Placer, Ana Cristina Lázaro-Callejón, Marina Maqueda, Mercedes Carrasco-Jimenez, María Paz Laso, Alejandro Aínsa, José A. Iglesias, Guillermo R. Perduca, Massimiliano López, Concepción Jiménez Pharmaceutics Article Among the strategies employed to overcome the development of multidrug-resistant bacteria, directed chemotherapy combined with local therapies (e.g., magnetic hyperthermia) has gained great interest. A nano-assembly coupling the antimicrobial peptide AS-48 to biomimetic magnetic nanoparticles (AS-48-BMNPs) was demonstrated to have potent bactericidal effects on both Gram-positive and Gram-negative bacteria when the antimicrobial activity of the peptide was combined with magnetic hyperthermia. Nevertheless, intracellular pathogens remain challenging due to the difficulty of the drug reaching the bacterium. Thus, improving the cellular uptake of the nanocarrier is crucial for the success of the treatment. In the present study, we demonstrate the embedding cellular uptake of the original nano-assembly into THP-1, reducing the toxicity of AS-48 toward healthy THP-1 cells. We optimized the design of PLGA[AS-48-BMNPs] in terms of size, colloidal stability, and hyperthermia activity (either magnetic or photothermal). The stability of the nano-formulation at physiological pH values was evaluated by studying the AS-48 release at this pH value. The influence of pH and hyperthermia on the AS-48 release from the nano-formulation was also studied. These results show a slower AS-48 release from PLGA[AS-48-BMNPs] compared to previous nano-formulations, which could make this new nano-formulation suitable for longer extended treatments of intracellular pathogens. PLGA[AS-48-BMNPs] are internalized in THP-1 cells where AS-48 is liberated slowly, which may be useful to treat diseases and prevent infection caused by intracellular pathogens. The treatment will be more efficient combined with hyperthermia or photothermia. MDPI 2022-12-08 /pmc/articles/PMC9785849/ /pubmed/36559238 http://dx.doi.org/10.3390/pharmaceutics14122744 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
Gaglio, Salvatore Calogero
Jabalera, Ylenia
Montalbán-López, Manuel
Millán-Placer, Ana Cristina
Lázaro-Callejón, Marina
Maqueda, Mercedes
Carrasco-Jimenez, María Paz
Laso, Alejandro
Aínsa, José A.
Iglesias, Guillermo R.
Perduca, Massimiliano
López, Concepción Jiménez
Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens
title Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens
title_full Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens
title_fullStr Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens
title_full_unstemmed Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens
title_short Embedding Biomimetic Magnetic Nanoparticles Coupled with Peptide AS-48 into PLGA to Treat Intracellular Pathogens
title_sort embedding biomimetic magnetic nanoparticles coupled with peptide as-48 into plga to treat intracellular pathogens
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9785849/
https://www.ncbi.nlm.nih.gov/pubmed/36559238
http://dx.doi.org/10.3390/pharmaceutics14122744
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