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首页> 外文期刊>Nature reviews Cancer >A Novel Delivery Method of Cyclovirobuxine D for Brain-Targeting: Chitosan Coated Nanoparticles Loading Cyclovirobuxine D by Intranasal Administration
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A Novel Delivery Method of Cyclovirobuxine D for Brain-Targeting: Chitosan Coated Nanoparticles Loading Cyclovirobuxine D by Intranasal Administration

机译:一种新型脑靶向环杂杂氨酸D的递送方法:壳聚糖涂层纳米颗粒加载烯烃基氧杂核酸

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The blood-brain barrier (BBB) restricts the delivery of most drugs to the brain. In our previous study, the feasibility of cyclovirobuxine D delivery to the brain by a non-invasive nasal route was evaluated. In this study, a suitable drug delivery system by way of intranasal administration was developed, which could improve brain targeting. First, a formulation of cyclovirobuxine D (CVB-D) based on chitosan nanoparticles (CS-CVB-D-NPs) was prepared by the modified ionotropic gelation method through single-factor screening experiment. The CS-CVB-D-NPs with a entrapment efficiency (EE) of (62.82 +/- 2.59)% were found to be of a narrow polydispersity index (PI) (0.19 +/- 0.01) and (235.37 +/- 12.71) nm in size, with a zeta potential of (33.9 +/- 1.7) mV. The NPs possessed a sustained release characterization with in vitro release of 88.03 +/- 2.30% at 24 h. In vivo, the higher AUC(0-t(brain)) of CS-CVB-D-NPs by intranasal administration revealed the development of a novel brain-targeting delivery method of CVB-D.
机译:血脑屏障(BBB)限制了大多数药物的递送给大脑。在我们以前的研究中,评估了通过非侵入性鼻途径向大脑的环杂杂软霉素D递送的可行性。在该研究中,开发了一种通过鼻内给药的合适的药物递送系统,可以改善脑靶向。首先,通过单因素筛选实验,通过改性的离子胶质凝胶化方法制备基于壳聚糖纳米颗粒(CS-CVB-D-NPS)的环杂核D(CVB-D)的制剂。发现具有(62.82 +/- 2.59)%(62.82 +/- 2.59)%的CS-CVB-D-NPS是狭窄的多分散指数(PI)(0.19 +/- 0.01)和(235.37 +/- 12.71 )尺寸为nm,具有(33.9 +/- 1.7)mV的Zeta电位。 NPS在24小时中具有88.03 +/- 2.30%的体外释放的持续释放表征。体内,通过鼻内给药的CS-CVB-D-NPS的较高AUC(脑))显示CVB-D的新型脑靶向递送方法的发展。

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