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纳米结构脂质载体(NLC)的肠溶包衣和填充 NLC 的硬明胶胶囊的肠溶包衣:可行性研究。

Enteric coating of nanostructured lipid carriers (NLCs) and enteric coating of hard gelatin capsules filled with NLCs: Feasibility studies.

机构信息

Department of Pharmaceutics, Manipal College of Pharmaceutical Sciences, Manipal University, Manipal, Karnataka State, India.

出版信息

Pak J Pharm Sci. 2021 Jul;34(4):1323-1331.

Abstract

Nanostructured lipid carriers (NLCs) of asenapine maleate (ASPM) were enteric coated with polymethacrylate polymers (Eudragit®) for oral delivery. The present study aimed to compare the feasibility of direct enteric coating of NLCs and enteric coating of hard gelatin capsules filled with lyophilized ASPM-NLCs. Organic solution of Eudragit® was prepared using acetone containing 3% v/v water, acetone or ethanol. Aqueous dispersion of Eudragit® was obtained by neutralization with base. Capsules were enteric coated by dip-coating method with 3:2 ratio of Eudragit® L100-55:S100 (7.5-12.5% w/v). ASPM-NLCs showed particle size of 84.91±2.14nm, polydispersity index of 0.222±0.026, entrapment efficiency of 86.9±1.8% and zeta potential of -4.83±0.29 mV. TEM images showed good sphericity of the particles with the size of ≈100nm. Non-aqueous enteric coating was not successful as NLCs were precipitated in organic solvent. Aqueous enteric coated ASPM-NLCs (lipid:coat=1:2) showed an increased size (150.8±16.7nm) and zeta potential (-23.5±2.2 mV) revealing the deposition of Eudragit®. However, aqueous enteric coated ASPM-NLCs and uncoated ASPM-NLCs showed higher drug release (18.3±3.1-22.3±3.2%) in HCl solution (pH 1.2) indicating no resistance offered by direct enteric coating of NLCs; whereas enteric coated capsules showed less drug release (4.7±0.8%) in HCl solution indicating sufficient gastric protection.

摘要

马来酸阿塞那平的纳米结构脂质载体 (NLC) 用聚甲基丙烯酸酯聚合物 (Eudragit®) 进行肠溶包衣,用于口服给药。本研究旨在比较直接肠溶包衣 NLC 和填充冻干 ASPM-NLC 的硬明胶胶囊肠溶包衣的可行性。使用含 3% v/v 水的丙酮制备 Eudragit® 的有机溶液,使用丙酮或乙醇。通过用碱中和获得 Eudragit® 的水性分散体。通过浸涂法用 Eudragit® L100-55:S100(7.5-12.5% w/v) 的 3:2 比例对胶囊进行肠溶包衣。ASPM-NLC 显示出 84.91±2.14nm 的粒径、0.222±0.026 的多分散指数、86.9±1.8%的包封效率和-4.83±0.29mV 的 zeta 电位。TEM 图像显示颗粒具有约 100nm 的良好球形度。非水肠溶包衣不成功,因为 NLC 在有机溶剂中沉淀。水性肠溶包衣的 ASPM-NLC(lipid:coat=1:2) 显示出增加的粒径 (150.8±16.7nm) 和 zeta 电位 (-23.5±2.2mV),表明 Eudragit® 的沉积。然而,水性肠溶包衣的 ASPM-NLC 和未包衣的 ASPM-NLC 在 HCl 溶液(pH 1.2)中显示出更高的药物释放(18.3±3.1-22.3±3.2%),表明 NLC 的直接肠溶包衣没有提供阻力; 而肠溶包衣胶囊在 HCl 溶液中显示出较少的药物释放(4.7±0.8%),表明胃有足够的保护。

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