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聚合物辅料对无定形氟康唑成核和晶体生长动力学的影响。

Effect of polymeric excipients on nucleation and crystal growth kinetics of amorphous fluconazole.

机构信息

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

出版信息

Biomater Sci. 2021 Jun 15;9(12):4308-4316. doi: 10.1039/d1bm00104c.

Abstract

Amorphous solids have been widely used to improve the solubility and oral bioavailability of poorly water-soluble drugs. Biocompatible polymeric materials are usually incorporated into formulations to inhibit the crystallization of high-energy amorphous drugs. Crystallization typically consists of two steps, nucleation and crystal growth. The impacts of polymeric excipients on the crystal growth of amorphous drugs have been intensively studied. However, the nucleation behaviors of amorphous drugs in the presence of polymers remain largely unexplored. Herein, we report that three chemically distinct polymers show significantly different effects on nucleation kinetics of amorphous fluconazole (FCZ), a classical antifungal drug. The addition of 10% w/w HPMCAS shows the largest inhibitory effect on the nucleation rates of FCZ, while the same amount of PVP has only a minor effect. Conversely, the nucleation rates for both polymorphs of FCZ are significantly increased in the presence of PEO. In addition, the polymeric additives are found to influence the kinetics of nucleation and crystal growth to a similar extent, suggesting that the two processes may share a similar kinetic barrier. The present study is helpful in the optimization of formulations of amorphous solid dispersions and understanding the nucleation behavior of polymorphic drugs.

摘要

无定形固体已被广泛用于提高低水溶性药物的溶解度和口服生物利用度。通常将生物相容性聚合物材料掺入制剂中以抑制高能无定形药物的结晶。结晶通常由成核和晶体生长两个步骤组成。聚合物辅料对无定形药物晶体生长的影响已得到深入研究。然而,聚合物存在下无定形药物的成核行为在很大程度上仍未得到探索。在此,我们报告三种化学性质不同的聚合物对经典抗真菌药物无定形氟康唑(FCZ)的成核动力学具有显著不同的影响。添加 10wt%羟丙甲纤维素琥珀酸酯(HPMCAS)对 FCZ 的成核速率具有最大的抑制作用,而相同量的聚乙烯吡咯烷酮(PVP)的影响则较小。相反,在 PEO 的存在下,FCZ 的两种多晶型物的成核速率都显著增加。此外,发现聚合物添加剂对成核和晶体生长动力学的影响程度相似,这表明这两个过程可能具有相似的动力学障碍。本研究有助于优化无定形固体分散体的配方,并理解多晶型药物的成核行为。

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