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Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles

Dacarbazine (DB) is an antineoplastic drug extensively used in cancer therapy. However, present limitations on its performance are related to its low solubility, instability, and non-specificity. To overcome these drawbacks, DB was included in β-cyclodextrin (βCD), which increased its aqueous solubi...

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Autores principales: Quintana-Contardo, Sebastián, Donoso-González, Orlando, Lang, Erika, Guerrero, Ariel R., Noyong, Michael, Simon, Ulrich, Kogan, Marcelo J., Yutronic, Nicolás, Sierpe, Rodrigo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9960602/
https://www.ncbi.nlm.nih.gov/pubmed/36839779
http://dx.doi.org/10.3390/pharmaceutics15020458
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author Quintana-Contardo, Sebastián
Donoso-González, Orlando
Lang, Erika
Guerrero, Ariel R.
Noyong, Michael
Simon, Ulrich
Kogan, Marcelo J.
Yutronic, Nicolás
Sierpe, Rodrigo
author_facet Quintana-Contardo, Sebastián
Donoso-González, Orlando
Lang, Erika
Guerrero, Ariel R.
Noyong, Michael
Simon, Ulrich
Kogan, Marcelo J.
Yutronic, Nicolás
Sierpe, Rodrigo
author_sort Quintana-Contardo, Sebastián
collection PubMed
description Dacarbazine (DB) is an antineoplastic drug extensively used in cancer therapy. However, present limitations on its performance are related to its low solubility, instability, and non-specificity. To overcome these drawbacks, DB was included in β-cyclodextrin (βCD), which increased its aqueous solubility and stability. This new βCD@DB complex has been associated with plasmonic gold nanoparticles (AuNPs), and polyethylene glycol (PEG) has been added in the process to increase the colloidal stability and biocompatibility. Different techniques revealed that DB allows for a dynamic inclusion into βCD, with an association constant of 80 M(−1) and a degree of solubilization of 0.023, where βCD showed a loading capacity of 16%. The partial exposure of the NH(2) group in the included DB allows its interaction with AuNPs, with a loading efficiency of 99%. The PEG-AuNPs-βCD@DB nanosystem exhibits an optical plasmonic absorption at 525 nm, a surface charge of −29 mV, and an average size of 12 nm. Finally, laser irradiation assays showed that DB can be released from this platform in a controlled manner over time, reaching a concentration of 56 μg/mL (43% of the initially loaded amount), which, added to the previous data, validates its potential for drug delivery applications. Therefore, the novel nanosystem based on βCD, AuNPs, and PEG is a promising candidate as a new nanocarrier for DB.
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spelling pubmed-99606022023-02-26 Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles Quintana-Contardo, Sebastián Donoso-González, Orlando Lang, Erika Guerrero, Ariel R. Noyong, Michael Simon, Ulrich Kogan, Marcelo J. Yutronic, Nicolás Sierpe, Rodrigo Pharmaceutics Article Dacarbazine (DB) is an antineoplastic drug extensively used in cancer therapy. However, present limitations on its performance are related to its low solubility, instability, and non-specificity. To overcome these drawbacks, DB was included in β-cyclodextrin (βCD), which increased its aqueous solubility and stability. This new βCD@DB complex has been associated with plasmonic gold nanoparticles (AuNPs), and polyethylene glycol (PEG) has been added in the process to increase the colloidal stability and biocompatibility. Different techniques revealed that DB allows for a dynamic inclusion into βCD, with an association constant of 80 M(−1) and a degree of solubilization of 0.023, where βCD showed a loading capacity of 16%. The partial exposure of the NH(2) group in the included DB allows its interaction with AuNPs, with a loading efficiency of 99%. The PEG-AuNPs-βCD@DB nanosystem exhibits an optical plasmonic absorption at 525 nm, a surface charge of −29 mV, and an average size of 12 nm. Finally, laser irradiation assays showed that DB can be released from this platform in a controlled manner over time, reaching a concentration of 56 μg/mL (43% of the initially loaded amount), which, added to the previous data, validates its potential for drug delivery applications. Therefore, the novel nanosystem based on βCD, AuNPs, and PEG is a promising candidate as a new nanocarrier for DB. MDPI 2023-01-30 /pmc/articles/PMC9960602/ /pubmed/36839779 http://dx.doi.org/10.3390/pharmaceutics15020458 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
Quintana-Contardo, Sebastián
Donoso-González, Orlando
Lang, Erika
Guerrero, Ariel R.
Noyong, Michael
Simon, Ulrich
Kogan, Marcelo J.
Yutronic, Nicolás
Sierpe, Rodrigo
Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles
title Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles
title_full Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles
title_fullStr Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles
title_full_unstemmed Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles
title_short Optimizing Dacarbazine Therapy: Design of a Laser-Triggered Delivery System Based on β-Cyclodextrin and Plasmonic Gold Nanoparticles
title_sort optimizing dacarbazine therapy: design of a laser-triggered delivery system based on β-cyclodextrin and plasmonic gold nanoparticles
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9960602/
https://www.ncbi.nlm.nih.gov/pubmed/36839779
http://dx.doi.org/10.3390/pharmaceutics15020458
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