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Nifedipine Nanoparticle Agglomeration as a Dry Powder Aerosol Formulation Strategy

机译:硝苯地平纳米颗粒团聚作为干粉气溶胶配制策略

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摘要

Efficient administration of drugs represents a leading challenge in pulmonary medicine. Dry powder aerosols are of great interest compared to traditional aerosolized liquid formulations in that they may offer improved stability, ease of administration, and simple device design. Particles 1–5 µm in size typically facilitate lung deposition. Nanoparticles may be exhaled as a result of their small size; however, they are desired to enhance the dissolution rate of poorly soluble drugs. Nanoparticles of the hypertension drug nifedipine were co-precipitated with stearic acid to form a colloid exhibiting negative surface charge. Nifedipine nanoparticle colloids were destabilized by using sodium chloride to disrupt the electrostatic repulsion between particles as a means to achieve the agglomerated nanoparticles of a controlled size. The aerodynamic performance of agglomerated nanoparticles was determined by cascade impaction. The powders were found to be well suited for pulmonary delivery. In addition, nanoparticle agglomerates revealed enhanced dissolution of the drug species suggesting the value of this formulation approach for poorly water soluble pulmonary medicines. Ultimately, nifedipine powders are envisioned as an approach to treat pulmonary hypertension.
机译:药物的有效给药代表了肺部医学的主要挑战。与传统的气雾化液体制剂相比,干粉气雾剂引起了极大的兴趣,因为它们可以提供更高的稳定性,易于给药和简单的装置设计。 1-5 µm的颗粒通常会促进肺部沉积。纳米粒子可能由于其较小的尺寸而被呼出。但是,它们需要提高难溶性药物的溶解速度。高血压药物硝苯地平的纳米颗粒与硬脂酸共沉淀,形成具有负表面电荷的胶体。通过使用氯化钠破坏颗粒之间的静电排斥力来使硝苯地平纳米颗粒胶体不稳定,以此作为获得可控制尺寸的团聚纳米颗粒的手段。通过级联碰撞测定团聚的纳米颗粒的空气动力学性能。发现这些粉末非常适合肺部递送。另外,纳米颗粒附聚物显示出药物种类的增强的溶解,这表明该制剂方法对于水溶性差的肺部药物的价值。最终,硝苯地平粉被设想为一种治疗肺动脉高压的方法。

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