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Crystallisation Behaviour of Pharmaceutical Compounds Confined within Mesoporous Silicon

机译:局限在中孔硅中的药物化合物的结晶行为

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摘要

The poor aqueous solubility of new and existing drug compounds represents a significant challenge in pharmaceutical development, with numerous strategies currently being pursued to address this issue. Amorphous solids lack the repeating array of atoms in the structure and present greater free energy than their crystalline counterparts, which in turn enhances the solubility of the compound. The loading of drug compounds into porous materials has been described as a promising approach for the stabilisation of the amorphous state but is dependent on many factors, including pore size and surface chemistry of the substrate material. This review looks at the applications of mesoporous materials in the confinement of pharmaceutical compounds to increase their dissolution rate or modify their release and the influence of varying pore size to crystallise metastable polymorphs. We focus our attention on mesoporous silicon, due to the ability of its surface to be easily modified, enabling it to be stabilised and functionalised for the loading of various drug compounds. The use of neutron and synchrotron X-ray to examine compounds and the mesoporous materials in which they are confined is also discussed, moving away from the conventional analysis methods.
机译:新药和现有药物化合物的水溶性差,代表了药物开发中的重大挑战,目前正在寻求众多策略来解决这一问题。非晶态固体缺乏结构中原子的重复排列,并且比其晶体对应物具有更大的自由能,这反过来又提高了化合物的溶解度。已经描述了将药物化合物装载到多孔材料中作为稳定无定形状态的一种有前途的方法,但是取决于许多因素,包括孔径和底物材料的表面化学性质。这篇综述着眼于介孔材料在限制药物化合物中的应用,以提高其溶解速率或改变其释放以及改变孔径以结晶亚稳多晶型物的影响。我们将注意力集中在中孔硅上,这是由于其表面易于修饰的能力,使其能够稳定并功能化以装载各种药物化合物。还讨论了使用中子和同步加速器X射线检查化合物及其所处的中孔材料的方法,从而摆脱了常规分析方法。

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