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Título : Combination Chemotherapy with Cisplatin and Chloroquine: Effect of Encapsulation in Micelles Formed by Self-Assembling Hybrid Dendritic–Linear–Dendritic Block Copolymers
Autor: González-Pastor, Rebeca ORCID SCOPUSID
Lancelot, Alexandre SCOPUSID
Morcuende-Ventura, Violeta SCOPUSID
San Anselmo, María SCOPUSID
Sierra, Teresa ORCID SCOPUSID
Serrano, José L. SCOPUSID
Martín-Duque, Pilar ORCID RESEARCHERID SCOPUSID
Palabras clave : Chloroquine; Cisplatin; Combination chemotherapy; Encapsulation; Hybrid dendritic– linear–dendritic block copolymers
Fecha de publicación: 14-may-2021
Editorial : MDPI
Citación : González-Pastor, R.; Lancelot, A.; Morcuende-Ventura, V.; San Anselmo, M.; Sierra, T.; Serrano, J.L.; Martin-Duque, P. Combination Chemotherapy with Cisplatin and Chloroquine: Effect of Encapsulation in Micelles Formed by Self-Assembling Hybrid Dendritic–Linear–Dendritic Block Copolymers. Int. J. Mol. Sci. 2021, 22, 5223. https://doi.org/10.3390/ijms22105223
Resumen : Clinical outcomes of conventional drug combinations are not ideal due to high toxicity to healthy tissues. Cisplatin (CDDP) is the standard component for many cancer treatments, yet its principal dose-limiting side effect is nephrotoxicity. Thus, CDDP is commonly used in combination with other drugs, such as the autophagy inhibitor chloroquine (CQ), to enhance tumor cell killing efficacy and prevent the development of chemoresistance. In addition, nanocarrier-based drug delivery systems can overcome chemotherapy limitations, decreasing side effects and increasing tumor accumulation. The aim of this study was to evaluate the toxicity of CQ and CDDP against tumor and non-tumor cells when used in a combined treatment. For this purpose, two types of micelles based on Pluronic® F127 hybrid dendritic–linear–dendritic block copolymers (HDLDBCs) modified with polyester or poly(esteramide) dendrons derived from 2,20 -bis(hydroxymethyl)propionic acid (HDLDBC-bMPA) or 2,20 -bis(glycyloxymethyl)propionic acid (HDLDBC-bGMPA) were explored as delivery nanocarriers. Our results indicated that the combined treatment with HDLDBC-bMPA(CQ) or HDLDBC-bGMPA(CQ) and CDDP increased cytotoxicity in tumor cells compared to the single treatment with CDDP. Encapsulations demonstrated less short-term cytotoxicity individually or when used in combination compared to the free drugs. However, and more importantly, a low degree of cytotoxicity against non-tumor cells was maintained, even when drugs were given simultaneously.
URI : https://repositorio.usj.es/handle/123456789/609
ISSN : 1661-6596
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