Magnetically induced drug release from niosome-based nanocarriers loaded with doxorubicin
Drake, Philip ; Amalina, I. ; Sari, R. ; ; Ramazan, S. ; Hope, G. ; Pancholi, D. ; Miatmoko, A.
Drake, Philip
Amalina, I.
Sari, R.
Ramazan, S.
Hope, G.
Pancholi, D.
Miatmoko, A.
Publication Date
2025-08
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This article is licensed under a Creative Commons Attribution 3.0 Unported Licence.
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2025-06-28
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Abstract
Niosomes co-loaded with doxorubicin and magnetic nanoparticles were synthesised using the thin film hydration method. The loading efficiency of the doxorubicin was between 60–70%. The hydrodynamic diameter measured as the average number (mean ± standard deviation), using dynamic light scattering, was found to be 188 ± 68 nm, 141 ± 86 nm and 169 ± 69 nm for the plain niosomes, niosomes loaded with doxorubicin and niosomes loaded with doxorubicin and magnetic nanoparticles, respectively. The zeta potential for all three niosome samples was determined to be −26.4 mV ± 1.9 mV. The thermally mediated release of doxorubicin was monitored using fluorescence spectroscopy and found to follow 1st order kinetics. The rate constant for the thermal release was 1.2 × 10−6, 1.0 × 10−4 and 5.1 × 10−4 min−1 at 298, 313 and 333 K, respectively. The doxorubicin was also released using an alternating magnetic field, this also followed 1st order kinetics and had a rate constant of 1.7 × 10−2 min−1. This is four orders of magnitude greater than the thermal release at the same temperature (298 K). The work shows the magnetically controlled, burst release from a drug-loaded niosome delivery system. The release was triggered on demand by the application of the alternating magnetic field, resulting in 86% doxorubicin release within 3 hours compared to 3% release in 30 days via thermal
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Drake P, Amalina I, Sari R et al (2025) Magnetically induced drug release from niosome-based nanocarriers loaded with doxorubicin. Soft Matter. 21: 6197-6206.
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