pH/Thermo-Responsive Grafted Alginate-Based SiO 2 Hybrid Nanocarrier/Hydrogel Drug Delivery Systems

We report the preparation of mesoporous silica nanoparticles covered by layer by layer (LbL) oppositely charged weak polyelectrolytes, comprising poly(allylamine hydrochloride) (PAH) and a sodium alginate, highly grafted by -isopropylacrylamide/ -tert-butylacrylamide random copolymers, NaALG-g-P(NIP...

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Published in:Polymers 2021-04, Vol.13 (8)
Main Authors: Theodorakis, Nikolaos, Saravanou, Sofia-Falia, Kouli, Nikoleta-Paraskevi, Iatridi, Zacharoula, Tsitsilianis, Constantinos
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container_title Polymers
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creator Theodorakis, Nikolaos
Saravanou, Sofia-Falia
Kouli, Nikoleta-Paraskevi
Iatridi, Zacharoula
Tsitsilianis, Constantinos
description We report the preparation of mesoporous silica nanoparticles covered by layer by layer (LbL) oppositely charged weak polyelectrolytes, comprising poly(allylamine hydrochloride) (PAH) and a sodium alginate, highly grafted by -isopropylacrylamide/ -tert-butylacrylamide random copolymers, NaALG-g-P(NIPAM NtBAM ) (NaALG-g). Thanks to the pH dependence of the degree of ionization of the polyelectrolytes and the LCST-type thermosensitivity of the grafting chains of the NaALG-g, the as-prepared hybrid nanoparticles (hNP) exhibit pH/thermo-responsive drug delivery capabilities. The release kinetics of rhodamine B (RB, model drug) can be controlled by the number of PAH/NaALG-g bilayers and more importantly by the environmental conditions, namely, pH and temperature. As observed, the increase of pH and/or temperature accelerates the RB release under sink conditions. The same NaALG-g was used as gelator to fabricate a hNP@NaALG-g hydrogel composite. This formulation forms a viscous solution at room temperature, and it is transformed to a self-assembling hydrogel (sol-gel transition) upon heating at physiological temperature provided that its T was regulated at 30.7 °C, by the NtBAM hydrophobic monomer incorporation in the side chains. It exhibits excellent injectability thanks to its combined thermo- and shear-responsiveness. The hNP@NaALG-g hydrogel composite, encapsulating hNP covered with one bilayer, exhibited pH-responsive sustainable drug delivery. The presented highly tunable drug delivery system (DDS) (hNP and/or composite hydrogel) might be useful for biomedical potential applications.
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Thanks to the pH dependence of the degree of ionization of the polyelectrolytes and the LCST-type thermosensitivity of the grafting chains of the NaALG-g, the as-prepared hybrid nanoparticles (hNP) exhibit pH/thermo-responsive drug delivery capabilities. The release kinetics of rhodamine B (RB, model drug) can be controlled by the number of PAH/NaALG-g bilayers and more importantly by the environmental conditions, namely, pH and temperature. As observed, the increase of pH and/or temperature accelerates the RB release under sink conditions. The same NaALG-g was used as gelator to fabricate a hNP@NaALG-g hydrogel composite. This formulation forms a viscous solution at room temperature, and it is transformed to a self-assembling hydrogel (sol-gel transition) upon heating at physiological temperature provided that its T was regulated at 30.7 °C, by the NtBAM hydrophobic monomer incorporation in the side chains. 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title pH/Thermo-Responsive Grafted Alginate-Based SiO 2 Hybrid Nanocarrier/Hydrogel Drug Delivery Systems
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