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蒙脱石和锂蒙脱石粘土材料在用于基本药物阿立哌唑的脂质制剂固化中的应用:体外和体内研究。

Montmorillonite and Laponite Clay Materials for the Solidification of Lipid-Based Formulations for the Basic Drug Blonanserin: In Vitro and in Vivo Investigations.

机构信息

Department of Science and Environment , Roskilde University , 4000 Roskilde , Denmark.

出版信息

Mol Pharm. 2018 Sep 4;15(9):4148-4160. doi: 10.1021/acs.molpharmaceut.8b00555. Epub 2018 Aug 14.

DOI:10.1021/acs.molpharmaceut.8b00555
PMID:30067372
Abstract

Solid-state lipid-based formulations offer great potential for the improved oral delivery of poorly water-soluble drugs. This study investigates the use of the high-surface-area clay materials, montmorillonite and laponite, as solid carriers for lipid-based formulations. The unique cation-exchange properties of clay platelets were exploited to preload the ionizable hydrophobic compound, blonanserin, prior to encapsulating a drug-loaded lipid solution. Thus, solid-state lipid-based formulations with dual-loading capabilities were developed and studied. These formulations were compared with simple clay-based lipid formulations, where blonanserin was loaded in the lipid phase only. The drug release behavior of all clay-based formulations was assessed during in vitro dissolution studies under simulated gastric conditions and in vitro fasting intestinal lipolysis studies. Montmorillonite- and laponite-based lipid formulations significantly reduced blonanserin solubilization relative to a control lipid solution and silica-lipid hybrid particles, owing to incomplete drug release from the clay cation-exchange sites. This phenomenon was replicated during in vivo pharmacokinetic studies, whereby the bioavailability of simple clay-based lipid formulations was decreased relative to controls. Importantly, the solid-state dual-loaded montmorillonite-based lipid formulation provided an optimal pharmacokinetic performance, achieving the same degree of bioavailability enhancement as the control lipid solution. These findings indicate the potential of solid-state dual-loaded clay-based lipid formulations for increasing drug loading levels and enhancing the oral absorption of poorly soluble weak base compounds.

摘要

固态脂质基制剂为改善难溶性药物的口服递送提供了巨大的潜力。本研究探讨了高比表面积粘土材料蒙脱石和皂土作为脂质基制剂的固体载体的应用。粘土片层的独特阳离子交换特性被利用,在包封载药脂质溶液之前预载可离子化的疏水性化合物,blonanserin。因此,开发并研究了具有双重载药能力的固态脂质基制剂。将这些制剂与仅在脂质相中载药的简单粘土基脂质制剂进行了比较。在模拟胃条件下的体外溶解研究和体外禁食肠脂肪分解研究中评估了所有基于粘土的制剂的药物释放行为。与对照脂质溶液和硅脂质杂化颗粒相比,蒙脱石和皂土基脂质制剂显著降低了 blonanserin 的溶解度,这是由于药物从粘土阳离子交换位不完全释放。这一现象在体内药代动力学研究中得到了复制,其中简单的粘土基脂质制剂的生物利用度相对于对照降低。重要的是,固态双重载药蒙脱石基脂质制剂提供了最佳的药代动力学性能,达到了与对照脂质溶液相同程度的生物利用度增强。这些发现表明,固态双重载药粘土基脂质制剂有潜力提高药物载药量并增强难溶性弱碱性化合物的口服吸收。

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