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万古霉素和克拉霉素多功能控释粒子的先进喷雾干燥设计、理化特性表征和干粉吸入气溶胶的气溶胶分散性能,用于靶向呼吸递药。

Advanced spray-dried design, physicochemical characterization, and aerosol dispersion performance of vancomycin and clarithromycin multifunctional controlled release particles for targeted respiratory delivery as dry powder inhalation aerosols.

机构信息

University of Kentucky, College of Pharmacy, Department of Pharmaceutical Sciences, Drug Development Division, Lexington, KY 40536-0596, USA.

出版信息

Int J Pharm. 2013 Oct 15;455(1-2):374-92. doi: 10.1016/j.ijpharm.2013.06.047. Epub 2013 Jun 29.

Abstract

Respirable microparticles/nanoparticles of the antibiotics vancomycin (VCM) and clarithromycin (CLM) were successfully designed and developed by novel organic solution advanced spray drying from methanol solution. Formulation optimization was achieved through statistical experimental design of pump feeding rates of 25% (Low P), 50% (Medium P) and 75% (High P). Systematic and comprehensive physicochemical characterization and imaging were carried out using scanning electron microscopy (SEM), hot-stage microscopy (HSM), differential scanning calorimetry (DSC), X-ray powder diffraction (XRPD), Karl Fischer titration (KFT), laser size diffraction (LSD), gravimetric vapor sorption (GVS), confocal Raman microscopy (CRM) and spectroscopy for chemical imaging mapping. These novel spray-dried (SD) microparticulate/nanoparticulate dry powders displayed excellent aerosol dispersion performance as dry powder inhalers (DPIs) with high values in emitted dose (ED), respirable fraction (RF), and fine particle fraction (FPF). VCM DPIs displayed better aerosol dispersion performance compared to CLM DPIs which was related to differences in the physicochemical and particle properties of VCM and CLM. In addition, organic solution advanced co-spray drying particle engineering design was employed to successfully produce co-spray-dried (co-SD) multifunctional microparticulate/nanoparticulate aerosol powder formulations of VCM and CLM with the essential lung surfactant phospholipid, dipalmitoylphosphatidylcholine (DPPC), for controlled release pulmonary nanomedicine delivery as inhalable dry powder aerosols. Formulation optimization was achieved through statistical experimental design of molar ratios of co-SD VCM:DPPC and co-SD CLM:DPPC. XRPD and DSC confirmed that the phospholipid bilayer structure in the solid-state was preserved following spray drying. Co-SD VCM:DPPC and co-SD CLM:DPPC dry powder aerosols demonstrated controlled release of antibiotic drug that was fitted to various controlled release mathematical fitting models. The Korsmeyer-Peppas model described the best data fit for all powders suggesting super case-II transport mechanism of controlled release. Excellent aerosol dispersion performance for all co-SD microparticulate/nanoparticulate DPIs was higher than the SD antibiotic drugs suggesting that DPPC acts as an aerosol performance enhancer for these antibiotic aerosol dry powders. Co-SD VCM:DPPC DPIs had higher aerosol dispersion parameters compared to co-SD CLM:DPPC which was related to differences in the physicochemical properties of VCM and CLM.

摘要

通过从甲醇溶液中进行新型有机溶液高级喷雾干燥,成功设计并开发了抗生素万古霉素(VCM)和克拉霉素(CLM)的可呼吸的微粒/纳米粒子。通过泵进料率为 25%(低 P)、50%(中 P)和 75%(高 P)的统计实验设计实现了配方优化。使用扫描电子显微镜(SEM)、热台显微镜(HSM)、差示扫描量热法(DSC)、X 射线粉末衍射(XRPD)、卡尔费休滴定(KFT)、激光粒度衍射(LSD)、重量法蒸汽吸附(GVS)、共焦拉曼显微镜(CRM)和化学成像映射进行了系统和全面的物理化学特性和成像研究。这些新型喷雾干燥(SD)的微粒/纳米颗粒干粉显示出作为干粉吸入剂(DPIs)的优异的气溶胶分散性能,具有高的发射剂量(ED)、可呼吸分数(RF)和细颗粒分数(FPF)。与 CLM DPIs 相比,VCM DPIs 显示出更好的气溶胶分散性能,这与 VCM 和 CLM 的物理化学和颗粒性质差异有关。此外,采用有机溶液高级共喷雾干燥颗粒工程设计,成功地生产了 VCM 和 CLM 与必需的肺表面活性剂磷脂二棕榈酰磷脂酰胆碱(DPPC)的共喷雾干燥(co-SD)多功能微粒/纳米颗粒气溶胶粉末制剂,用于作为可吸入干粉气溶胶的受控释放肺纳米药物传递。通过 co-SD VCM:DPPC 和 co-SD CLM:DPPC 的共喷雾干燥摩尔比的统计实验设计实现了配方优化。XRPD 和 DSC 证实,喷雾干燥后固体状态中的磷脂双层结构得以保留。co-SD VCM:DPPC 和 co-SD CLM:DPPC 干粉气溶胶显示出抗生素药物的控释,该药物拟合各种控释数学拟合模型。Korsmeyer-Peppas 模型描述了所有粉末的最佳数据拟合,表明控释的超二级传输机制。所有 co-SD 微粒/纳米颗粒 DPIs 的优异的气溶胶分散性能均高于 SD 抗生素药物,表明 DPPC 是这些抗生素气溶胶干粉的气溶胶性能增强剂。与 co-SD CLM:DPPC 相比,co-SD VCM:DPPC DPIs 具有更高的气溶胶分散参数,这与 VCM 和 CLM 的物理化学性质差异有关。

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