Nanovesicular Formulation of Brimonidine Tartrate for the Management of Glaucoma: In Vitro and In Vivo Evaluation

被引:0
|
作者
Sabyasachi Maiti
Sayon Paul
Ranjit Mondol
Somasree Ray
Biswanath Sa
机构
[1] Gupta College of Technological Sciences,Department of Pharmaceutical Technology, Centre for Advanced Research in Pharmaceutical Sciences
[2] Division of Pharmaceutics,undefined
[3] Ashram More,undefined
[4] Jadavpur University,undefined
来源
AAPS PharmSciTech | 2011年 / 12卷
关键词
entrapment efficiency; hypotensive activity; nanovesicles; ocular drug delivery; release kinetics;
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学科分类号
摘要
In this study, nanovesicles were developed for brimonidine tartrate by film hydration technique and dispersed in viscous carbopol solution for ocular delivery. Scanning electron microscopy revealed spherical shape of the vesicles. As high as 32.27% drug entrapment efficiency was achieved depending upon the surfactant/cholesterol molar ratio (7:4 to 7:8). The vesicles were in the size range of 298.0–587.9 nm. Release study showed a biphasic drug-release pattern for the lyophilized vesicular formulation in buffered saline solution, i.e., initial burst release followed by gradual release over the period of 8 h. On contrary, the isolated vesicles reduced the burst effect in 3 h by two to three times and the drug release was comparatively slower at the intermediate ratio in both cases. With variation in cholesterol content, the drug release followed either first order or Higuchi’s kinetics. Physically the lyophilized vesicular formulations were more stable at refrigerated temperature. DSC and X-RD analyses indicated loss of drug crystallinity in the vesicles. FTIR spectroscopy did not reveal any interaction between drug and excipients. The lyophilized formulation showed better ocular hypotensive activity than marketed drops on albino rabbits and in vivo efficacy was sustained up to 7.5 h. Furthermore, the formulation was found to be non-irritant to the rabbit eye. Hence, the lyophilized vesicles, when dispersed in viscous carbopol solution, had the potential in reducing dosing frequency and could improve patient compliance.
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页码:755 / 763
页数:8
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