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西咪替丁、尼扎替丁和法莫替丁等无定形药物中的慢弛豫动力学

The Slow Relaxation Dynamics in the Amorphous Pharmaceutical Drugs Cimetidine, Nizatidine, and Famotidine.

作者信息

Viciosa M Teresa, Moura Ramos Joaquim J, Diogo Hermínio P

机构信息

Centro de Química-Física Molecular and Institute of Nanoscience and Nanotechnology, Instituto Superior Técnico, Universidade de Lisboa, Lisboa, Portugal.

Centro de Química Estrutural, Complexo I, Instituto Superior Técnico, Universidade de Lisboa, Lisboa, Portugal.

出版信息

J Pharm Sci. 2016 Dec;105(12):3573-3584. doi: 10.1016/j.xphs.2016.08.019. Epub 2016 Oct 20.

Abstract

The slow molecular mobility in the amorphous solid state of 3 active pharmaceutical drugs (cimetidine, nizatidine, and famotidine) has been studied using differential scanning calorimetry and the 2 dielectric-related techniques of dielectric relaxation spectroscopy and thermally stimulated depolarization currents. The glass-forming ability, the glass stability, and the tendency for crystallization from the equilibrium melt were investigated by differential scanning calorimetry, which also provided the characterization of the main relaxation of the 3 glass formers. The chemical instability of famotidine at the melting temperature and above it prevented the preparation of the amorphous for dielectric studies. In contrast, for cimetidine and nizatidine, the dielectric study yielded the main kinetic features of the α relaxation and of the secondary relaxations. According to the obtained results, nizatidine displays the higher fragility index of the 3 studied glass-forming drugs. The thermally stimulated depolarization current technique has proved useful to identify the Johari-Goldstein relaxation and to measure τ in the amorphous solid state, that is, in a frequency range which is not easily accessible by dielectric relaxation spectroscopy.

摘要

利用差示扫描量热法以及介电弛豫光谱和热刺激去极化电流这两种与介电相关的技术,研究了3种活性药物(西咪替丁、尼扎替丁和法莫替丁)在非晶态固体状态下缓慢的分子迁移率。通过差示扫描量热法研究了玻璃形成能力、玻璃稳定性以及从平衡熔体中结晶的倾向,该方法还对3种玻璃形成体的主要弛豫进行了表征。法莫替丁在熔点及以上温度时的化学不稳定性阻碍了用于介电研究的非晶体制备。相比之下,对于西咪替丁和尼扎替丁,介电研究得出了α弛豫和次级弛豫的主要动力学特征。根据所得结果,尼扎替丁在所研究的3种玻璃形成药物中表现出更高的脆性指数。热刺激去极化电流技术已被证明有助于识别乔哈里-戈尔茨坦弛豫并测量非晶态固体状态下的τ,即在介电弛豫光谱不易达到的频率范围内。

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