Issue 16, 2024, Issue in Progress

pH-responsive niosome-based nanocarriers of antineoplastic agents

Abstract

Differences in pH between the tumour interstitium and healthy tissues can be used to induce conformational changes in the nanocarrier structure, thereby triggering drug release at the desired site. In the present study, novel pH-responsive nanocarriers were developed by modifying conventional niosomes with hexadecyl-poly(acrylic acid)n copolymers (HD-PAAn). Niosomal vesicles were prepared by the thin film hydration method using Span 60, Span 60/Tween 60 and cholesterol as main constituents, and HD-PAA modifiers of different concentrations (0.5, 1, 2.5, 5 mol%). Next, two model substances, a water-soluble fluorescent dye (calcein) and a hydrophobic agent with pronounced antineoplastic activity (curcumin), were loaded in the aqueous core and hydrophobic membrane of the elaborated niosomes, respectively. Physicochemical properties of blank and loaded nanocarriers such as hydrodynamic diameter (Dh), size distribution, zeta potential, morphology and pH-responsiveness were investigated in detail. The cytotoxicity of niosomal curcumin was evaluated against human malignant cell lines of different origins (MJ, T-24, HUT-78), and the mechanistic aspects of proapoptotic effects were elucidated. The formulation composed of Span 60/Tween 60/cholesterol/2.5% HD-PAA17 exhibited optimal physicochemical characteristics (Dh 302 nm; ζ potential −22.1 mV; high curcumin entrapment 83%), pH-dependent drug release and improved cytotoxic and apoptogenic activity compared to free curcumin.

Graphical abstract: pH-responsive niosome-based nanocarriers of antineoplastic agents

Supplementary files

Article information

Article type
Paper
Submitted
21 Feb 2024
Accepted
01 Apr 2024
First published
11 Apr 2024
This article is Open Access
Creative Commons BY-NC license

RSC Adv., 2024,14, 11124-11140

pH-responsive niosome-based nanocarriers of antineoplastic agents

V. Gugleva, R. Mihaylova, G. Momekov, K. Kamenova, A. Forys, B. Trzebicka, M. Petrova, I. Ugrinova, D. Momekova and P. D. Petrov, RSC Adv., 2024, 14, 11124 DOI: 10.1039/D4RA01334D

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