What does this research mean for the field?

Polymeric matrix mini-tablets based on Eudragit® S 100 and HPMC provide a robust platform for the controlled release of pantoprazole, protecting it during gastric exposure and enabling pH-dependent release in the intestine. Novelty: ClaimNovelty.NOVEL_FINDING. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

The aim is to develop a polymeric matrix mini-tablet formulation for pantoprazole that protects it in acidic conditions and allows for controlled release in the intestine.

March 7, 2026Open Access

Polymeric Matrix Mini-Tablets Based on Eudragit® S 100 and HPMC for Controlled Release of Pantoprazole

Key Points

The aim is to develop a polymeric matrix mini-tablet formulation for pantoprazole that protects it in acidic conditions and allows for controlled release in the intestine.
Blended pantoprazole with excipients to create formulations.
Compressed blends into mini-tablets using an eccentric tablet press.
Conducted dissolution studies under varying pH conditions.
Employed analytical techniques like HPLC and DSC for characterization.
Analyzed drug release kinetics using mathematical models.
Formulations F2 and F6 showed effective gastro-resistant performance and sustained release up to 24 hours.
Kinetic modeling revealed formulation-dependent drug release mechanisms.
Physico-mechanical attributes influenced drug-release behavior, as shown by multivariate analysis.

Abstract

Background: Pantoprazole is a widely used proton pump inhibitor that is highly unstable under acidic conditions. This limits the performance of conventional formulations and typically requires enteric-coated dosage forms or alternative modified-release approaches. This study reports the development of polymeric matrix mini-tablets designed to protect pantoprazole during gastric exposure and to enable pH-dependent release under intestinal conditions. The formulations combine Eudragit® S 100, a pH-dependent polymer, with HPMC, a hydrophilic matrix former that modulates drug release through hydration and swelling. Methods: Matrix mini-tablets were prepared by blending pantoprazole with selected excipients at optimised proportions and compressing the blends by direct compression using an eccentric tablet press. Powder blends and mini-tablets were characterised according to pharmacopoeial specifications. Analytical techniques—including High-Performance Liquid Chromatography (HPLC), Differential Scanning Calorimetry (DSC), Fourier-Transform Infrared Absorption Spectroscopy (FT-IR), Powder X-Ray Diffraction (PXRD), and Scanning Electron Microscopy (SEM)—were employed to evaluate drug content uniformity, thermal behaviour, and potential drug–excipient interactions. In vitro dissolution studies were performed under sequential pH conditions, and the release kinetics were analysed using mathematical models. Results: Dissolution testing identified formulations F2 and F6 as providing the most suitable gastro-resistant performance in the acidic stage, together with sustained release up to 24 h. Kinetic modelling supported formulation-dependent release mechanisms, and multivariate analysis (PCA) highlighted relationships between physico-mechanical attributes and drug-release behaviour. Conclusions: The proposed matrix system shows potential as a robust, coating-free platform for the modified delivery of acid-labile drugs using direct compression, simplifying manufacturing. These findings support the rational design of oral modified-release formulations based on polymeric matrices.

Polymeric Matrix Mini-Tablets Based on Eudragit® S 100 and HPMC for Controlled Release of Pantoprazole

Key Points

Abstract

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