The granules were passed through #16. These granules were lubricated with magnesium stearate and talc and compressed into tablet on low compression force on 10 station
punching machine using 8 mm punches. Table 1. Composition of cefdinir floating GSK2118436 in vivo layer of bilayer tablet. The in vitro buoyancy behavior was characterized by floating lag time and total floating time (n = 6). The test was performed using USP 23 dissolution apparatus II was 900 ml of 0.1 N HCl at paddle speed 75 rpm at 37 °C ± 0.5 °C. The time required for the tablet to rise to the surface of the dissolution medium and the duration of time the tablet constantly floated on the dissolution medium were noted as floating lag time and total buoyancy time, respectively.
14 and 15 The dimensional stability and in vitro dissolution of the formulations was studied using USP 23 dissolution Apparatus II for the period of 24 h. The dissolution medium was 900 ml of 0.1 N HCL (1.2 pH). The temperature was maintained at 37 ± 0.5 °C at 50 rpm. The dimensional stability of cefdinir formulations were observed visually16 and in dissolution studies10 ml of aliquot were withdrawn at predetermined time intervals of each and every hour. The medium was replaced with 10 ml of fresh 0.1 N HCl each time. Sample was analyzed by using UV spectrophotometry at 276 nm. The dissolution profile of all the batches was fitted to zero order, first order,17 and 18 Higuchi,19, 20 and 21 Hixon and Crowell22 and Korsmeyer and Peppas11, 23, 24 and 25 using R-analysis. FTIR spectra of drug, placebo tablet (with all excipients except drug) and optimized CBT were Obeticholic Acid ic50 obtained on a JASCO FTIR 5300, Japan. Samples were prepared by mixing with KBr and placing in the sample holder. The samples were scanned from 4000 to 500 cm−1. Stability studies were performed according to ICH and WHO guidelines. Optimized CBT formulations were strip packed in laboratory in aluminum foil with polyethylene lamination and various replicates
Mannose-binding protein-associated serine protease were kept in the humidity chamber maintained at 45 °C and 75% RH and 37 °C for 3 months. At the end of studies, samples were analyzed for the drug content, in vitro dissolution, floating behavior and dimensional stability.26, 27 and 28 Cefdinir oral bioavailability has been reported to be 20–30% perhaps because of the poor absorption in the upper part of gastrointestinal tract. Gastroretentive drug delivery is one approach; in it, the GI residence time is prolonged because of the floating behavior of CBT were formulated for the immediate and sustained release action of dosage form. First, the matrix layer or floating layer was prepared and evaluated on the basis of floating behavior studies. It contains the effervescent mixture and different matrix forming polymers to retain the carbon dioxide produced from the effervescent mixture. Then the loading layer was developed on the basis of effervescent release of loading dose.