Cholesterol-functionalized carvedilol-loaded PLGA nanoparticles: anti-inflammatory, antioxidant, and antitumor effects

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作者
Ana Luiza C. de S. L. Oliveira
Alaine M. dos Santos-Silva
Arnóbio A. da Silva-Júnior
Vinícius B. Garcia
Aurigena A. de Araújo
Lioe-Fee de Geus-Oei
Alan B. Chan
Luis J. Cruz
Raimundo F. de Araújo Júnior
机构
[1] Federal University of Rio Grande do Norte (UFRN),Postgraduate Program in Health Science
[2] Leiden University Medical Center,Department of Radiology Translational Nanobiomaterials and Imaging
[3] Federal University of Rio Grande do Norte (UFRN),Department of Pharmacy Laboratory of Pharmaceutical Technology and Biotechnology
[4] Federal University of Rio Grande do Norte (UFRN),Department of Biophysics Postgraduate Programs in Public Health and Pharmaceutical Science and Pharmacology
[5] Leiden University Medical Center,Department of Radiology Nuclear Medicine
[6] Percuros B.V.,Department of Morphology Postgraduate Program in Functional and Structural Biology
[7] Federal University of Rio Grande do Norte (UFRN),undefined
来源
Journal of Nanoparticle Research | 2020年 / 22卷
关键词
Cancer; Inflammation; Oxidative stress; Colloidal nanocarriers; Functionalized nanoparticles; Drug delivery systems; Nanomedicine;
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摘要
The inflammation has been identified as factor of tumor progression, which has increased the interest and use of molecules with anti-inflammatory and antioxidant activities in the cancer treatment. In this study, the antioxidant, anti-inflammatory, and antitumor potentials of carvedilol was explored in a different approach. The cholesterol (CHO) was investigated as facilitated agent in the action of carvedilol-loaded nanoparticles. Different formulations exhibited spherical and stable nanoparticle with mean diameter size < 250 nm. The cholesterol changed the copolymer-drug interactions and the encapsulation efficiency. The in vitro cancer study was performed using murine colorectal cancer cell line (CT-26) to observe the cell viability and apoptosis on MTS assay and flow cytometry, respectively. The experiments have demonstrated that cholesterol improved the performance of drug-loaded nanoparticles, which was much better than free drug. The in vivo inflammation peritonitis model revealed that carvedilol-loaded nanoparticles increased the level of glutathione and leukocyte migration mainly when the functionalized drug-loaded nanoparticles were tested, in a lower dose than the free drug. As hypothesized, the experimental data suggest that cholesterol-functionalized carvedilol-loaded PLGA nanoparticles can be a novel and promising approach in the inflammation-induced cancer therapy since showed anti-inflammatory, antioxidant, and antitumor effects.
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