首页> 外文期刊>International Journal of Pharmaceutics >Application of Box-Behnken experimental design for the formulation and optimisation of selenomethionine-loaded chitosan nanoparticles coated with zein for oral delivery
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Application of Box-Behnken experimental design for the formulation and optimisation of selenomethionine-loaded chitosan nanoparticles coated with zein for oral delivery

机译:BATH-BEHNKEN试验设计在乳蛋白甲基硫醚加载的壳聚糖纳米粒子涂覆蛋白口服递送时的应用

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摘要

Selenomethionine is an essential amino acid with a narrow therapeutic index and susceptibility to oxidation. Here it was encapsulated into a nanoparticle composed of chitosan cross-linked with tripolyphosphate for oral delivery. The formulation was optimised using a three-factor Box-Behnken experimental design. The chitosan: tripolyphosphate ratio, chitosan solvent pH, and drug load concentration were independently varied. The dependent variables studied were encapsulation efficiency, particle size, polydispersity index and zeta potential. For optimisation, encapsulation efficiency and zeta potential were maximised, particle diameter was set to 300 nm and polydispersity index was minimised. A 0.15 mg/mL concentration of selenomethionine, chitosan solvent pH of 3, and chitosan: tripolyphosphate ratio of 6:1 yielded optimum nanoparticles of size 187 +/- 58 nm, polydispersity index 0.24 +/- 0.01, zeta potential 36 +/- 6 mV, and encapsulation efficiency of 39 +/- 3%. Encapsulation efficiency was doubled to 80 +/- 1.5% by varying pH of the ionotropic solution components and by subsequent coating of the NPs with zein, increasing NP diameter to 377 +/- 47 nm, whilst retaining polydispersity index and zeta potential values. Selenomethionine-entrapped nanoparticles were not cytotoxic to intestinal and liver cell lines. Accelerated thermal stability studies indicated good stability of the nanoparticles under normal storage conditions (23 degrees C). In simulated gastrointestinal and intestinal fluid conditions, 60% cumulative release was obtained over 6 h.
机译:Selenomethionine是一种必需的氨基酸,具有狭窄的治疗指数和氧化敏感性。在这里,它被包封成由与三聚磷酸三聚磷酸盐交联的壳聚糖组成的纳米颗粒。使用三因素Box-Behnken实验设计进行了优化。壳聚糖:三聚磷酸盐比,壳聚糖溶剂pH和药物负荷浓度独立变化。所研究的依赖变量是封装效率,粒度,多分散指数和Zeta电位。为了优化,封装效率和ζ电位最大化,粒径设定为300nm,并且最小化多分散性指数。 0.15mg / ml浓度的硒甲硫氨酸,壳聚糖溶剂pH为3,壳聚糖:三聚磷酸盐比为6:1,产生最佳纳米粒径为187 +/- 58nm,多分散指数0.24 +/- 0.01,Zeta电位36 +/- 6 mV,封装效率为39 +/- 3%。通过不同的离子溶液组分和随后用玉米蛋白涂覆NP,将NP直径增加至377 +/- 47nm,将封装效率加倍加倍80 +/- 1.5%。保持多分散指数和Zeta电位值。 Selenomethionine-捕获的纳米粒子不是肠道和肝细胞系的细胞毒性。加速热稳定性研究表明在正常储存条件下纳米颗粒的良好稳定性(23℃)。在模拟胃肠和肠道液条件下,在6小时内获得60%的累积释放。

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