PHARMACOKINETIC STUDIES OF RANITIDINE TABLETS ON HEALTHY HUMAN SUBJECTS USING TWO BINDERS
Akhtar, N., Ahmad, M., Aziz, G., Khan, H., Aleem, M., Mahmood, A. (2006). PHARMACOKINETIC STUDIES OF RANITIDINE TABLETS ON HEALTHY HUMAN SUBJECTS USING TWO BINDERS. EKB Journal Management System, 29(2), 416-431. doi: 10.21608/bfsa.2006.65220
N. Akhtar; M. Ahmad; G. Aziz; Haji M. S. Khan; M. Aleem; A. Mahmood. "PHARMACOKINETIC STUDIES OF RANITIDINE TABLETS ON HEALTHY HUMAN SUBJECTS USING TWO BINDERS". EKB Journal Management System, 29, 2, 2006, 416-431. doi: 10.21608/bfsa.2006.65220
Akhtar, N., Ahmad, M., Aziz, G., Khan, H., Aleem, M., Mahmood, A. (2006). 'PHARMACOKINETIC STUDIES OF RANITIDINE TABLETS ON HEALTHY HUMAN SUBJECTS USING TWO BINDERS', EKB Journal Management System, 29(2), pp. 416-431. doi: 10.21608/bfsa.2006.65220
Akhtar, N., Ahmad, M., Aziz, G., Khan, H., Aleem, M., Mahmood, A. PHARMACOKINETIC STUDIES OF RANITIDINE TABLETS ON HEALTHY HUMAN SUBJECTS USING TWO BINDERS. EKB Journal Management System, 2006; 29(2): 416-431. doi: 10.21608/bfsa.2006.65220

PHARMACOKINETIC STUDIES OF RANITIDINE TABLETS ON HEALTHY HUMAN SUBJECTS USING TWO BINDERS

Bulletin of Pharmaceutical Sciences Assiut University
Article 12, Volume 29, Issue 2, December 2006, Page 416-431  XML PDF (250.73 K)
Document Type: Original Article
DOI: 10.21608/bfsa.2006.65220
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Authors
N. Akhtar1; M. Ahmad1; G. Aziz1; Haji M. S. Khan2; M. Aleem3; A. Mahmood4
1Department of Pharmacy, Faculty of Pharmacy and Alternative Medicine, The Islamia University of Bahawalpur, PAKISTAN
2Department of Pharmacy, Hamdard University, Islamabad Campus, Islamabad, PAKISTAN
3Department of Statistics, Faculty of Science, The Islamia University of Bahawalpur, PAKISTAN
4College of Pharmacy, University of the Punjab, Lahore, PAKISTAN
Abstract
Ranitidine is an effective H2 receptor antagonist. Ranitidine is a specific, long acting H2 receptor antagonist. It is indicated for the treatment of duodenal ulcer, gastric ulcer, GERD and ZollingerEllison syndrome. In this study two formulations of Ranitidine 300 mg tablets were prepared and film coated. Starch and poly vinyl pyrolidone were used as binding agents to check the effect of the binding materials on the pharmacokinetic parameters of Ranitidine tablets. Different in vitro tests were used to evaluate Ranitidine tablets like disintegration test and dissolution test. Then in vivo evaluation was performed on these two formulations. Tablets were administered to eight normal human subjects comprising of two groups, each group consisted of four normal human subjects one by one in a crossover manner after one week washout period. Blood samples were collected and plasma was obtained and analyzed by HPLC. Statistical analysis was performed and the values for Cmax for formulation 1 were found to be 4.63 ± 0.47 µg/ml, and for formulation 2 it was 4.76 ± 1.02 µg/ml. The value for Tmax for formulation 1 was found to be 2.0 ± 0.37 hours, and for formulation 2 it was 1.5 ± 0.46 hours. The value for AUC for formulation 1 was found to be 18.57 ± 6.122 µg/hr/ml and for formulation 2 it was 26.43 ±22.38 µg/hr/ml. It was also concluded that different binders affect the bioavailability of the tablets and Ranitidine tablets prepared by polyvinyl pyrolidine have better bioavailability than those tablets prepared by starch as binding agent.
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