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无定形药物纳米混悬液。3. 颗粒溶解与晶体生长。

Amorphous drug nanosuspensions. 3. Particle dissolution and crystal growth.

作者信息

Lindfors Lennart, Skantze Pia, Skantze Urban, Westergren Jan, Olsson Ulf

机构信息

Pharmaceutical and Analytical R&D, AstraZeneca R&D Mölndal, Sweden.

出版信息

Langmuir. 2007 Sep 11;23(19):9866-74. doi: 10.1021/la700811b. Epub 2007 Aug 15.

Abstract

In the present paper, we have studied particle dissolution and crystal growth of the poorly water soluble drug felodipine, using fluorescence as a probe for the amount of crystalline material. Dissolution kinetics is essentially diffusion-controlled, while the rate of crystal growth is significantly slower compared to the diffusion-controlled limit. The deviation from diffusion control was characterized by the effective length, lambda, related to the kinetics of a surface integration process. Amorphous nanoparticles may be highly unstable in the presence of small amounts of crystalline particles. This is due to the fact that the molecular solubility from the amorphous nanoparticles often is at least an order of magnitude higher than the corresponding crystalline solubility. In a mixed system where crystalline nanoparticles have been added to an amorphous nanosuspension, the bulk will have a monomer concentration intermediate between the amorphous and crystalline solubilities, and is thus supersaturated with respect to the crystalline particles while being undersaturated with respect to the amorphous particles. As a consequence, the amorphous particles spontaneously dissolve, while crystalline particles grow, in a combined process which is similar to Ostwald ripening. By knowing the parameters describing dissolution and crystal growth, respectively, it was possible to simulate the outcome of controlled seeding experiments, where a small amount of crystalline nanoparticles was added to a dispersion of amorphous nanoparticles. A good agreement between model calculations and experiments was obtained including how the crystal growth rate varied with the amounts of added crystalline seeds.

摘要

在本论文中,我们以荧光作为结晶物质含量的探针,研究了难溶性药物非洛地平的颗粒溶解和晶体生长。溶解动力学本质上是扩散控制的,而晶体生长速率与扩散控制极限相比显著较慢。与扩散控制的偏差通过与表面整合过程动力学相关的有效长度λ来表征。在存在少量结晶颗粒的情况下,无定形纳米颗粒可能非常不稳定。这是因为无定形纳米颗粒的分子溶解度通常比相应的结晶溶解度至少高一个数量级。在将结晶纳米颗粒添加到无定形纳米悬浮液的混合体系中,整体的单体浓度将介于无定形和结晶溶解度之间,因此相对于结晶颗粒是过饱和的,而相对于无定形颗粒是不饱和的。结果,无定形颗粒自发溶解,而结晶颗粒生长,这是一个类似于奥斯特瓦尔德熟化的联合过程。通过分别了解描述溶解和晶体生长的参数,有可能模拟控制晶种实验的结果,即在无定形纳米颗粒分散体中添加少量结晶纳米颗粒的实验。模型计算与实验之间取得了良好的一致性,包括晶体生长速率如何随添加的结晶晶种量而变化。

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