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Research Article

Development of enteric submicron particles formulation of α-amylase for oral delivery

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Pages 560-569 | Received 31 Dec 2010, Accepted 27 Jun 2011, Published online: 26 Aug 2011
 

Abstract

Enteric submicron particles (SPs) formulations of α-amylase were prepared by w/o/w emulsion solvent evaporation using hydroxypropyl methylcellulose phthalate (HPMCP) and Eudragit L 100, to avoid gastric inactivation of α-amylase. Smaller internal and external aqueous phase volume provided maximum encapsulation efficiency (71.92–73.40%), least particle size (546.4–595.4 nm) and 23–26% loss of enzyme activity. Release studies in 0.1 N HCl confirmed the gastro-resistance of formulations. The anionic SPs aggregated in 0.1 N HCl (i.e. gastric pH 1.2), due to protonation of carboxylic groups of enteric polymer. The aggregates being < 500 µm size would not impede gastric emptying. However, at pH >5.0 (duodenal pH), SPs showed de-aggregation due to restoration of surface charge. HPMCP and Eudragit L 100 SPs facilitated almost complete release of α-amylase within 30 min at pH 6.0 and 6.8, respectively, following Higuchi kinetics. PXRD and DSC indicated amorphous character and scanning electron microscope showed spherical shape of SPs. In simulated gastro-intestinal pH condition, HPMCP and Eudragit L 100 SPs showed good digestion of cooked rice and could serve as potential carrier for oral enzyme delivery. Stability studies indicated the formulations as quite stable to ensure 2 years shelf life at room temperature.

Acknowledgments

The authors are thankful to Banasthali Vidhyapith, Rajasthan, India for providing facilities for the research. Thanks are also due, to Jubilant Organosys (Noida, India) for gifting enteric polymers (HPMCP and Eudragit L 100) and SAIF at AIIMS (New Delhi) for SEM.

Declaration of interest

The authors report no declarations of interest.

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