Optimized Chitosan-Coated Gliadin Nanoparticles Improved the Hesperidin Cytotoxicity over Tumor Cells

Kelte Filho, Irineo; Machado, Christiane Schineider; Diedrich, Camila; Karam, Thaysa Ksiaskiewcz; Nakamura, Celso Vataru; Khalil, Najeh Maissar; Mainardes, Rubiana Mara

doi:10.1590/1678-4324-75years-2021200795

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Article - 75 years - Special Edition • Braz. arch. biol. technol. 64 (spe) • 2021 • https://doi.org/10.1590/1678-4324-75years-2021200795 copy

Optimized Chitosan-Coated Gliadin Nanoparticles Improved the Hesperidin Cytotoxicity over Tumor Cells

Authorship SCIMAGO INSTITUTIONS RANKINGS

HIGHLIGHTS

A Taguchi design optimized the development of hesperidin-loaded gliadin nanoparticles.

A chitosan-coating was added to improve the physical stability of nanoparticles.

Nanoparticles reduced the hesperidin cytotoxicity over healthy Vero cells.

Nanoparticles improved the hesperidin cytotoxicity over tumor cells.

Abstract

Hesperidin is a natural compound which is found in citric fruits and presents antitumor and antimicrobial activities. However, the in vivo efficacy of Hesperidin is reduced due to its low oral bioavailability. Protein-based nanoparticles have been applied to improve biological parameters of drugs and natural compounds. Gliadin is a monomeric protein present in wheat. In this study, gliadin-based nanoparticles containing hesperidin were obtained by desolvation technique and a Taguchi orthogonal array design was employed to optimize the formulation. The independent variables were set as concentration of CaCl₂ (0.5; 1 or 2%) and stabilizing agent (Pluronic F68, Tween 80 or sodium caseinate). The dependent variables consisted of mean diameter, polydispersity index, zeta potential, and encapsulation efficiency. The results showed significant effects on the dependent variables when 1% CaCl₂ and Pluronic F68 were used. The optimized formulation was coated with chitosan to increase the physical stability of the nanoparticles. The final nanoparticles presented a mean diameter of 321 nm and polydispersity index of 0.217, and spherical shape. After coating, the Zeta potential was +21 mV, and the encapsulation efficiency was 73 %. The in vitro release assay showed that about 98% of the drug was released from the nanoparticles after 48 h. Moreover, the nanoparticles reduced hesperidin cytotoxicity on healthy cells (Vero cells) and improved the cytotoxicity on tumor cells (HeLa, PC-3 and Caco-2 cells). Results showed that the chitosan-coated gliadin nanoparticles are potential carriers for hesperidin delivery for cancer treatment.

Keywords:
Protein nanoparticles; Taguchi orthogonal array design; cytotoxicity

Experiment	Mean diameter (nm)	PDI	Zeta potential (mV)	EE (%)
1 (C1,S1)	179.60 ± 23.32	0.25 ± 0.12	-7.43 ± 0.55	50.84 ± 5.06
2 (C1,S2)	177.90 ± 22.55	0.28 ± 0.13	-8.07 ± 0.52	58.02 ± 5.07
3 (C1,S3)	1857.50 ± 337.70	0.53 ± 0.04	-13.10 ± 2.21	87.21 ± 4.71
4 (C2,S1)	226.50 ± 30.97	0.09 ± 0.02	-2.91 ± 0.68	80.11 ± 1.15
5 (C2,S2)	2253.00 ± 262.70	0.69 ± 0.20	-14.90 ± 1.41	49.74 ± 0.83
6 (C2,S3)	1659.50 ± 481.00	0.64 ± 0.09	-11.2 ± 3.11	83.21 ± 0.79
7 (C3,S1)	257.40 ± 25.72	0.16 ± 0.55	-0.21 ± 0.01	55.26 ± 3.01
8 (C3,S2)	1415.60 ± 143.21	0.75 ± 0.18	-14.70 ± 3.23	58.25 ± 8.50
9 (C3,S3)	2591.20 ± 355.80	0.78 ± 0.02	-12.30 ± 2.61	80.04 ± 2.04

Nanoparticles	Mean size (nm)	PDI	Zeta potential (mV)	EE (%)
GLINP-HES	226.50 ± 30.97^a	0.09 ± 0.02^a	-2.91 ± 0.68^a	80.11 ± 1.15^a
CHGLINP-HES	321.40 ± 39.60^b	0.217 ± 0.06^b	+21.40 ± 2.07^b	73.10 ± 2.42^b

Cell line	IC₅₀ (µg/mL)
Cell line	Free Hesperidin	CSGLINP-HES	Blank nanoparticles
Vero	230.83 ± 20.05	> 1000	> 1000
HeLa	70.44 ± 7.72	16 ± 1.61	159.33 ± 12.10
PC-3	179.05 ± 3.68	21.62 ± 1.84	126.67 ± 14.05
Caco-2	265.53 ± 17.56	164.87 ± 14.72	674.45 ± 62.03

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[1] *Correspondence: mainardes@unicentro.br; Tel.: +55-42-36298160 (R.M.M.).