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喷雾干燥药物纳米颗粒无定形结构的稳定化

Stabilization of the Amorphous Structure of Spray-Dried Drug Nanoparticles.

作者信息

Amstad Esther, Spaepen Frans, Weitz David A

机构信息

Institute of Materials, Ecole Polytechnique Fédérale de Lausanne (EPFL) , Lausanne CH-1015, Switzerland.

出版信息

J Phys Chem B. 2016 Sep 1;120(34):9161-5. doi: 10.1021/acs.jpcb.6b05417. Epub 2016 Aug 17.

Abstract

The bioavailability of hydrophobic drugs strongly increases if they are formulated as amorphous materials because the solubility of the amorphous phase is much higher than that of the crystal. Moreover, the stability of these particles against crystallization during storage increases with decreasing particle size. Hence, it is advantageous to formulate poorly water soluble drugs as amorphous nanoparticles. The formulation of an amorphous structure is often difficult because many of these drugs have a high propensity to crystallize. This difficulty can be overcome if drugs are spray-dried using a microfluidic nebulator we recently developed. However, these nanoparticles agglomerate when they come in contact with each other, and this compromises the stability of their amorphous structure through crystallization. To improve their stability, we coat the nanoparticles with a sterically stabilizing polymer layer; this can be accomplished by co-spraying them with an excipient. However, this excipient must meet strict solubility limits, which severely limit the choice of polymers. Alternatively, the nanoparticles can be sterically stabilized by spraying them directly into a polymeric matrix; this enables a much wider choice of stabilizing polymers.

摘要

如果将疏水性药物制成无定形材料,其生物利用度会显著提高,因为无定形相的溶解度远高于晶体。此外,这些颗粒在储存过程中抗结晶的稳定性会随着粒径的减小而增加。因此,将水溶性差的药物制成无定形纳米颗粒是有利的。形成无定形结构通常很困难,因为许多这类药物极易结晶。如果使用我们最近开发的微流控雾化器对药物进行喷雾干燥,这个难题是可以克服的。然而,这些纳米颗粒相互接触时会发生团聚,这会通过结晶破坏其无定形结构的稳定性。为了提高其稳定性,我们用空间稳定聚合物层包裹纳米颗粒;这可以通过将它们与辅料共同喷雾来实现。然而,这种辅料必须满足严格的溶解度限制,这严重限制了聚合物的选择。或者,可以通过将纳米颗粒直接喷雾到聚合物基质中来实现空间稳定;这使得稳定聚合物的选择范围更广。

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