Pharmacokinetics of colon-specific pH and time-dependent flurbiprofen tablets

Present research deals with the development of compression-coated flurbiprofen colon-targeted tablets to retard the drug release in the upper gastro intestinal system, but progressively release the drug in the colon. Flurbiprofen core tablets were prepared by direct compression method and were compression coated using sodium alginate and Eudragit S100. The formulation is optimized based on the in vitro drug release study and further evaluated by X-ray imaging and pharmacokinetic studies in healthy humans for colonic delivery. The optimized formulation showed negligible drug release (4.33 +/- A 0.06 %) in the initial lag period followed by progressive release (100.78 +/- A 0.64 %) for 24 h. The X-ray imaging in human volunteers showed that the tablets reached the colon without disintegrating in the upper gastrointestinal tract. The C (max) of colon-targeted tablets was 12,374.67 ng/ml at T (max) 10 h, where as in case of immediate release tablets the C (max) was 15,677.52 ng/ml at T (max) 3 h, that signifies the ability of compression-coated tablets to target the colon. Development of compression-coated tablets using combination of time-dependent and pH-sensitive approaches was suitable to target the flurbiprofen to colon.