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Phospholipid-stabilized nanoparticles of cyclosporine a by rapid expansion from supercritical to aqueous solution

机译:从超临界到水溶液的快速膨胀,磷脂稳定化的环孢素a纳米颗粒

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摘要

The purpose of this research was to form stable suspensions of submicron particles of cyclosporine A, a water-insoluble drug, by rapid expansion from supercritical to aqueous solution (RESAS). A solution of cyclosporine A in CO2 was expanded into an aqueous solution containing phospholipid vesicles mixed with nonionic surfactants to provide stabilization against particle growth resulting from collisions in the expanding jet. The products were evaluated by measuring drug loading with high performance liquid chromatography (HPLC), particle sizing by dynamic light scattering (DLS), and particle morphology by transmission electron microscopy (TEM) and x-ray diffraction. The ability of the surfactant molecules to orient at the surface of the particles and provide steric stabilization could be manipulated by changing process variables including temperature and suspension concentration. Suspensions with high payloads (up to 54 mg/mL) could be achieved with a mean diameter of 500 nm and particle size distribution ranging from 40 to 920 nm. This size range is several hundred nanometers smaller than that produced by RESAS for particles stabilized by Tween 80 alone. The high drug payloads (≈10 times greater than the equilibrium solubility), the small particle sizes, and the long-term stability make this process attractive for development.
机译:这项研究的目的是通过从超临界溶液到水溶液(RESAS)的快速膨胀,形成水不溶性药物环孢菌素A的亚微米颗粒的稳定悬浮液。将环孢菌素A在CO2中的溶液膨胀到含有磷脂囊泡和非离子表面活性剂混合的水溶液中,以提供稳定的稳定性,以防止膨胀喷嘴中的碰撞引起的颗粒生长。通过使用高效液相色谱(HPLC)测量药物载量,通过动态光散射(DLS)测量颗粒大小以及通过透射电子显微镜(TEM)和X射线衍射测量颗粒形态来评估产品。表面活性剂分子定向在颗粒表面并提供空间稳定的能力可以通过改变包括温度和悬浮液浓度在内的过程变量来控制。具有高有效负载量(最高54 mg / mL)的悬浮液的平均直径为500 nm,粒径分布范围为40至920 nm。该尺寸范围比RESAS为单独使用Tween 80稳定的颗粒所产生的尺寸范围小数百纳米。药物有效载荷高(比平衡溶解度大10倍左右),小粒径和长期稳定性,使该方法具有开发吸引力。

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