从生物分子和生物仿制药环境中分离药物:光谱和量热研究

IF 2.5 Q3 CHEMISTRY, PHYSICAL
Rahul Yadav, Bijan Kumar Paul, S. Mukherjee
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引用次数: 0

摘要

药物与核酸、蛋白质、脂质、氨基酸和其他生物受体的结合对于药物的运输是必要的。然而,如果结合的药物分子没有从载体上解离,特别是在无毒剂的帮助下,也可能产生各种副作用。因此,与生物分子结合的小药物分子的螯合是应对药物过量和药物解毒相关问题的核心。在这篇文章中,我们旨在介绍几种在体外实验条件下用于解离与不同生物和仿生组件结合的小药物分子的方法。为此,已经讨论了各种分子组装体的应用,如胶束、混合胶束、分子容器,如β-环糊精、葫芦[7]脲水合物等。在此,我们还试图通过光谱和量热技术揭示这种螯合过程背后的驱动力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Sequestration of Drugs from Biomolecular and Biomimicking Environments: Spectroscopic and Calorimetric Studies
The binding of drugs to nucleic acids, proteins, lipids, amino acids, and other biological receptors is necessary for the transportation of drugs. However, various side effects may also originate if the bound drug molecules are not dissociated from the carrier, especially with the aid of non-toxic agents. The sequestration of small drug molecules bound to biomolecules is thus central to counter issues related to drug overdose and drug detoxification. In this article, we aim to present several methods used for the dissociation of small drug molecules bound to different biological and biomimicking assemblies under in vitro experimental conditions. To this effect, the application of various molecular assemblies, like micelles, mixed micelles, molecular containers, like β-cyclodextrin, cucurbit[7]uril hydrate, etc., has been discussed. Herein, we also try to shed light on the driving forces underlying such sequestration processes through spectroscopic and calorimetric techniques.
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来源期刊
Colloids and Interfaces
Colloids and Interfaces CHEMISTRY, PHYSICAL-
CiteScore
3.90
自引率
4.20%
发文量
64
审稿时长
10 weeks
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