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低浓度聚环氧乙烷对吲哚美辛多晶型选择性加速生长。

Selective Acceleration of Crystal Growth of Indomethacin Polymorphs by Low-Concentration Poly(ethylene oxide).

机构信息

State Key Laboratory of Natural Medicines, Department of Pharmaceutics, China Pharmaceutical University , Nanjing 210009, China.

Department of Polymer Science and Engineering, School of Chemistry and Chemical Engineering, Nanjing University , Nanjing 210093, China.

出版信息

Mol Pharm. 2017 Dec 4;14(12):4694-4704. doi: 10.1021/acs.molpharmaceut.7b00854. Epub 2017 Nov 21.

Abstract

Physical stability of pharmaceutical amorphous solid dispersions is one of the critical attributes to the successful development of the formulation. Herein, we studied the impact of low-concentration poly(ethylene oxide) (PEO) on the crystallization rates of three polymorphs of indomethacin (IMC, γ-, α-, and δ-form). We observed that the addition of 3% w/w PEO significantly increased the crystal growth rates of γ-form and α-form of IMC, but had a negligible effect on the δ-form. The reduction of the activation energy for the crystal growth of IMC polymorphs after adding the PEO follows the order γ-form > α-form > δ-form, which is consistent with the trend toward the accelerating effects of PEO on the crystal growth rates of three polymorphs. With the addition of low-concentration PEO, there is an increase of molecular mobility of IMC as evidenced by the decreased structural relaxation times and viscosities. This study suggests that the substantially different effects of PEO on the crystal growth rates of IMC polymorphs are attributable to the different adsorption of PEO on the crystal surface of those polymorphs, which in turn exerts a selective accelerating effect on IMC molecules to organize into the different crystalline phases. These findings are relevant for understanding the crystallization behavior of amorphous solid dispersions containing polymorphic drugs.

摘要

药物无定形固体分散体的物理稳定性是制剂成功开发的关键属性之一。在此,我们研究了低浓度聚环氧乙烷(PEO)对吲哚美辛(IMC,γ-、α-和 δ-晶型)三种多晶型物结晶速率的影响。我们观察到,添加 3%w/w PEO 显著增加了 IMC γ-和 α-晶型的晶体生长速率,但对 δ-晶型的影响可以忽略不计。添加 PEO 后,IMC 多晶型物的晶体生长活化能降低的顺序为 γ-型>α-型>δ-型,这与 PEO 对三种多晶型物晶体生长速率的加速作用趋势一致。随着低浓度 PEO 的添加,IMC 的分子迁移率增加,这表现为结构弛豫时间和粘度的降低。这项研究表明,PEO 对 IMC 多晶型物晶体生长速率的显著不同影响归因于 PEO 在这些多晶型物晶体表面的不同吸附,这反过来对 IMC 分子施加了选择性的加速作用,使其组织成不同的晶相。这些发现对于理解含有多晶型药物的无定形固体分散体的结晶行为具有重要意义。

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