论文信息 - Gamma scintigraphic evaluation of film-coated tablets intended for colonic or biphasic release.

Gamma scintigraphic evaluation of film-coated tablets intended for colonic or biphasic release.

The gastrointestinal transit and in vivo drug release behaviour of a film-coated tablet formulation was investigated in five healthy human subjects using the technique of gamma scintigraphy. The film coating system consisted of a mixture of pectin, chitosan and HPMC in a ratio of 6:1:0.37 applied to 750 mg cores at a coat weight gain of 9%. The estimated mean values of the gastric emptying time (62+/-17 min), small intestinal transit time (219+/-53 min), ileocaecal junction lag time (79+/-30 min) and the colon arrival time (345+/-33 min), were similar to published values for the transit of similar sized tablets in humans. The amount of radioactive tracer released from the labelled tablets was minimal when the tablets were in the stomach and the small intestine. There was increased release of radioactivity when the tablets were in the colon due to increased degradation of the film coatings by pectinolytic enzymes resident in the colon. The pectin/chitosan/HPMC film coating system thus acts as a colonic delivery system.

[1] S. S. Davis,et al. Gastrointestinal transit of dosage forms in the pig , 2001, The Journal of pharmacy and pharmacology.

[2] R. Brunelle,et al. Gastric emptying of enteric-coated tablets , 1984, Digestive Diseases and Sciences.

[3] K. Ofori-Kwakye,et al. Biphasic drug release from film-coated tablets. , 2003, International journal of pharmaceutics.

[4] G. Macleod,et al. Selective drug delivery to the colon using pectin:chitosan:hydroxypropyl methylcellulose film coated tablets. , 1999, International journal of pharmaceutics.

[5] K. Ofori-Kwakye,et al. Biphasic drug release: the permeability of films containing pectin, chitosan and HPMC. , 2001, International journal of pharmaceutics.

[6] S. S. Davis,et al. The use of gamma scintigraphy to follow the gastrointestinal transit of pharmaceutical formulations , 1985, The Journal of pharmacy and pharmacology.

[7] P. Kamath,et al. Motility of the ileocolonic junction. , 1988, Gut.

[8] I. Wilding,et al. The role of γ-scintigraphy in oral drug delivery , 1991 .

[9] M. Alpsten,et al. Gastro-intestinal transit of a multiple-unit formulation (metoprolol CR/ZOK) and a non-disintegrating tablet with the emphasis on colon , 1996 .

[10] K. Yuen,et al. Gamma-scintigraphic study of the gastrointestinal transit and in vivo dissolution of a controlled release diclofenac sodium formulation in xanthan gum matrices. , 2000, International journal of pharmaceutics.