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首页> 外文期刊>Science of advanced materials >Development and Optimization of Carteolol Loaded Carboxymethyl Tamarind Kernel Polysaccharide Nanoparticles for Ophthalmic Delivery: Box-Behnken Design, In Vitro, Ex Vivo Assessment
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Development and Optimization of Carteolol Loaded Carboxymethyl Tamarind Kernel Polysaccharide Nanoparticles for Ophthalmic Delivery: Box-Behnken Design, In Vitro, Ex Vivo Assessment

机译:卡特洛尔负载的羧甲基罗望子碱羧甲基核仁多糖纳米颗粒的开发和优化:Box-Behnken设计,体外,离体评估

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In the present study, three level and two factor Box-Behnken statistical experimental design was used to optimize the carteolol loaded carboxymethyl tamarind kernel polysaccharide nanoparticles (CMKP) formulation for ocular delivery system. The effects of three independent parameters like polymer concentration, calcium chloride (CaCl_2) concentration (crosslinking agent) and sonication time were studied on dependent variables like particle size and entrapment efficiency. The fitted mathematical model allowed us to plot response surfaces curves and to determine optimal preparation conditions. Results clearly indicated that polymer concentration and crosslinking agent were the main factor influencing particle size and entrapment efficiency. Optimization was done by point prediction of software and the concentrations which were found to be optimum i.e., carboxymethyl tamarind kernel polysaccharide (0.15% w/v), CaCl_2 (0.20% w/v), and sonication time (30 min) with 223.66 ±3.56 nm particle size and 38.32 ±2.14% entrapment efficiency. The nanoparticles were characterized for in vitro release and transcorneal permeation study which revealed sustained release and significant permeation (P = 0.0058) as compared to pure drug solution. The nanoparticles were also characterized for bioadhesion, irritation study (Hen Egg Test-Chorioallantoic Membrane, HET-CAM), confocal microscopy and histopathology study and the results showed that the formulation could be prepared successfully promising their use in ocular delivery.
机译:在本研究中,使用三级和两因素Box-Behnken统计实验设计来优化卡特洛尔负载的羧甲基罗望子仁核仁多糖纳米颗粒(CMKP)制剂的眼部递送系统。研究了三个独立参数(如聚合物浓度,氯化钙(CaCl_2)浓度(交联剂)和超声处理时间)对诸如粒径和包封率等因变量的影响。拟合的数学模型使我们能够绘制响应面曲线并确定最佳制备条件。结果清楚地表明,聚合物浓度和交联剂是影响粒径和包封率的主要因素。通过软件的点预测进行优化,发现最佳浓度,即羧甲基罗望子果仁多糖(0.15%w / v),CaCl_2(0.20%w / v)和超声处理时间(30分钟),为223.66± 3.56 nm粒径和38.32±2.14%的包封率。纳米粒子的特点是用于体外释放和角膜渗透研究,与纯药物溶液相比,该研究显示了持续释放和显着渗透(P = 0.0058)。还对纳米颗粒进行了生物粘附,刺激性研究(Hen Egg Test-尿囊化膜,HET-CAM),共聚焦显微镜和组织病理学研究,结果表明该制剂可以成功制备,有望用于眼部递送。

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