Pharmacokinetic study of repaglinide floating drug delivery system in rabbits by RP-HPLC method

doi:10.5246/jcps.2012.02.021

Pharmacokinetic study of repaglinide floating drug delivery system in rabbits by RP-HPLC method

T. Ramanjireddy^*, D. Dhachinamoorthi, K.B. Chandrasekhar

1. Department of Pharmaceutics, CES College of Pharmacy, Kurnool 518218, India
2. Department of Pharmaceutics, QIS College of Pharmacy, Ongole 523002, India
3. Department of Chemistry, JNTUA, Anantapur 515002, India

收稿日期:2011-09-16 修回日期:2011-12-12 出版日期:2012-03-15 发布日期:2012-03-15
通讯作者: T. Ramanjireddy*

Pharmacokinetic study of repaglinide floating drug delivery system in rabbits by RP-HPLC method

T. Ramanjireddy^*, D. Dhachinamoorthi, K.B. Chandrasekhar

1. Department of Pharmaceutics, CES College of Pharmacy, Kurnool 518218, India
2. Department of Pharmaceutics, QIS College of Pharmacy, Ongole 523002, India
3. Department of Chemistry, JNTUA, Anantapur 515002, India

Received:2011-09-16 Revised:2011-12-12 Online:2012-03-15 Published:2012-03-15
Contact: T. Ramanjireddy*

摘要/Abstract

摘要： The present work is aimed to study the pharmacokinetic parameters of optimized repaglinide floating drug delivery system (FDDS) by 2⁴ factorial designs, followed by comparison with a commercially available formulation. The main effects and interactions of formulation variables were studied by using normal and pareto charts. The optimized formulation shows a fickian diffusion drug release mechanism. Pharmacokinetic parameters of the designed drug delivery system were evaluated in rabbit models. Mean while a simple, specific high performance liquid chromatographic method was developed and validated as per biopharmaceutical specifications, the linearity was observed at the range of 110-550 ng/mL (r² = 0.999). By using methanol-phosphate buffer (pH 2.5) (70:30, v/v) as mobile phase at the flow rate of 1.0 mL/min the validation shows a better retention time of 5.2 min for repaglinide. And the same validation method was used for pharmacokinetic profile analysis of repaglinide marketed products and FDDS. The comparative pharmacokinetic results such as t_max, half-life, area under the curve, mean residence times were increased significantly for the repaglinide in FDDS than the marketed product of repaglinide except C_max and elimination rate constant.

关键词: Pharmacokinetic study, Floating drug delivery system, Rabbit model

Abstract: The present work is aimed to study the pharmacokinetic parameters of optimized repaglinide floating drug delivery system (FDDS) by 2⁴ factorial designs, followed by comparison with a commercially available formulation. The main effects and interactions of formulation variables were studied by using normal and pareto charts. The optimized formulation shows a fickian diffusion drug release mechanism. Pharmacokinetic parameters of the designed drug delivery system were evaluated in rabbit models. Mean while a simple, specific high performance liquid chromatographic method was developed and validated as per biopharmaceutical specifications, the linearity was observed at the range of 110-550 ng/mL (r² = 0.999). By using methanol-phosphate buffer (pH 2.5) (70:30, v/v) as mobile phase at the flow rate of 1.0 mL/min the validation shows a better retention time of 5.2 min for repaglinide. And the same validation method was used for pharmacokinetic profile analysis of repaglinide marketed products and FDDS. The comparative pharmacokinetic results such as t_max, half-life, area under the curve, mean residence times were increased significantly for the repaglinide in FDDS than the marketed product of repaglinide except C_max and elimination rate constant.

Key words: Pharmacokinetic study, Floating drug delivery system, Rabbit model

中图分类号:

R969.1

Supporting: ^*Corresponding author. Tel.: +91-7382106566

T. Ramanjireddy^*, D. Dhachinamoorthi, K.B. Chandrasekhar. Pharmacokinetic study of repaglinide floating drug delivery system in rabbits by RP-HPLC method [J]. , DOI: 10.5246/jcps.2012.02.021.

[1]	陈彦安, 周心怡, 张文魁, 许光阳^* . 液相色谱串联质谱法测定人体血浆中非索非那定含量及其药代动力学研究[J]. , 2013, 22(5): 409-414.
[2]	李艳姣, 刘慧敏, 党晓芳, 张硕峰, 吴金英, 贾占红, 韩立炜^*. HPLC方法研究葛根素混合胶束在Beagle犬体内的药代动力学[J]. , 2012, 21(4): 327-332.
[3]	李梦瑶1,2, 吴琼2, 李汉青2, 宁妙然2, 陈烨2, 李良1,2, 周田彦1,2, 卢炜1,2. 液质联用法同时测定埃罗替尼及其活性代谢产物OSI-420在BALB/c裸鼠体内的浓度及其药代动力学研究[J]. , 2012, 21(4): 296-303.
[4]	陈烨, 李汉青, 许娇娇, 酒向飞, 邓晨辉, 李新刚, 李良, 徐小晴, 周田彦^, 卢炜^. 高效液相离子对色谱法测定糖尿病大鼠血浆中二甲双胍浓度及其药代动力学研究[J]. , 2012, 21(3): 211-218.
[5]	黄慧莲, 刘科兰, 邵峰, 任刚, 叶耀辉, 张寿文, 刘荣华^*. 高效液相-质谱串联方法快速测定大鼠血浆中的槲皮素-3'-O-葡萄糖苷含量[J]. , 2012, 21(3): 219-225.
[6]	李叶桓, 张国州, 黄荣华, 李冬冬, 罗钰, 杨勇, 吴银群, 刘丽慧, 曾慧慧^*. 新型有机硒类抗肿瘤化合物WB硒啉在体内组织分布研究[J]. , 2011, 20(6): 578-583.
[7]	孙晓利, 刘东华, 李鹏, 徐文方, 张娜^* . 静脉注射用乌苯美司脂肪乳制备及药代动力学研究[J]. , 2011, 20(5): 483-492.
[8]	孙立新^*, 陈扬, 杨雯雯, 郭君阳, 赵挺, 佟立今. RP-HPLC-UV法测定大鼠血浆中西瑞香素浓度[J]. , 2011, 20(5): 493-497.
[9]	闫冲, 林励^*, 刘红菊, 张延娇, 陈雅慧. HPLC研究异牡荆苷在大鼠体内的药代动力学及组织分布[J]. , 2011, 20(4): 376-382.
[10]	张静, 张蕊, 魏春敏, 袁桂艳, 刘晓燕, 王本杰, 郭瑞臣^*. LC-MS/MS测定人血浆中甘草次酸的浓度及其在药代动力学中的应用[J]. , 2011, 20(4): 383-389.
[11]	柳文媛, 杨晓静, 冯锋^*, 徐晓珍. 代谢产物鉴定及汉黄芩素与汉黄芩素-7-O-葡萄糖醛酸苷的同时测定: 小鼠肝脏的分布研究[J]. , 2011, 20(3): 282-289.
[12]	李汉青, 陈烨, 李载权, 邓晨辉, 李良, 毕姗姗, 李梦瑶, 周田彦^, 卢炜^. 高效液相色谱法测定肿瘤模型BALB/c裸鼠血浆中埃罗替尼的浓度及其药代动力学研究[J]. , 2011, 20(3): 245-252.
[13]	马廷升^*, 李高, 杨光忠, 刘志华, 朱兰寸. 盐酸特拉唑嗪口服渗透泵控释片人体药物动力学研究[J]. , 2011, 20(3): 253-258.
[14]	杨琳, 郭晓宇^, 王齐放, 陈颖, 车亦馨, 车庆明^. 大鼠血清中黄芩素代谢产物的鉴定[J]. , 2011, 20(3): 275-281.
[15]	刘亚欧, 范洁明, 王学清^*, 张强. 索拉非尼自微乳化给药系统的制备及药物动力学研究[J]. , 2011, 20(2): 164-170.

Pharmacokinetic study of repaglinide floating drug delivery system in rabbits by RP-HPLC method

Pharmacokinetic study of repaglinide floating drug delivery system in rabbits by RP-HPLC method

PDF (PC)

可视化

摘要/Abstract

引用本文

使用本文

参考文献

相关文章 15

编辑推荐

Metrics

本文评价