Advanced interpenetrating polymer networks for innovative gastroretentive formulations targeting Helicobacter pylori gastric colonization
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Abstract
The escalating challenges of Helicobacter pylori-induced gastric complications, driven by rising antibiotic resistance
and persistent cancer risks, underscore the demand for innovative therapeutic strategies. This study addresses
this urgency through the development of tailored semi-interpenetrating polymer networks (semi-IPN)
serving as gastroretentive matrices for amoxicillin (AMOX). They are biodegradable, absorb significant volume of
simulated gastric fluid (swelling index > 360 %) and exhibit superporous microstructures, remarkable
mucoadhesion, and buoyancy. The investigation includes assessment at pH 1.2 for comparative analysis with
prior studies and, notably, at pH 5.0, reflecting the acidic environment in H. pylori-infected stomachs. The semi-
IPN demonstrated gel-like structures, maintaining integrity throughout the 24-hour controlled release study, and
disintegrating upon completing their intended function. Evaluated in gastroretentive drug delivery system performance,
AMOX release at pH 1.2 and pH 5.0 over 24 h (10 %-100 %) employed experimental design methodology,
elucidating dominant release mechanisms. Their mucoadhesive, buoyant, three-dimensional scaffold
stability, and gastric biodegradability make them ideal for accommodating substantial AMOX quantities.
Furthermore, exploring the inclusion of the potassium-competitive acid blocker (P-CAB) vonoprazan (VONO) in
AMOX-loaded formulations shows promise for precise and effective drug delivery. This innovative approach has
the potential to combat H. pylori infections, thereby preventing the gastric cancer induced by this pathogen.
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Bibliographic citation
Grosso, R., Benito, E., Carbajo-Gordillo, A. I., Díaz, M. J., García-Martín, M. G., & de-Paz, M.-V. (2024). Advanced interpenetrating polymer networks for innovative gastroretentive formulations targeting Helicobacter pylori gastric colonization. In European Journal of Pharmaceutical Sciences (Vol. 200, p. 106840). Elsevier BV. https://doi.org/10.1016/j.ejps.2024.106840














