化学
生物相容性
体内
生物分子
生物物理学
药物输送
碳酸氢盐
纳米技术
磷酸盐
粉末衍射
化学工程
结晶学
生物化学
有机化学
材料科学
生物技术
工程类
生物
作者
Michael A. Luzuriaga,Candace Benjamin,M. Gaertner,Hamilton Lee,Fabian C. Herbert,Snipta Mallick,Jeremiah J. Gassensmith
标识
DOI:10.1080/10610278.2019.1616089
摘要
The emergence of drug delivery using water stable metal-organic frameworks has elicited a lot of interest in their biocompatibility. However, few studies have been conducted on their stability in common buffers, cell media, and blood proteins. For these studies, single crystal ZIF-8 approximately 1 um in diameter were synthesized, incubated with common laboratory buffers, cell media, and serum, and then characterized by PXRD, IR, DLS, and SEM. Time-resolved SEM and PXRD demonstrate that buffers containing phosphate and bicarbonate alter the appearance and composition of ZIF-8; however, cargo inside the ZIF-8 does not appear to leak out, in most of these buffers, even when the ZIF-8 itself is displaced by phosphates. On the other hand, blood proteins in serum dissolve ZIF-8, causing trapped biomolecules to escape. The study presented here suggests that ZIF-8 can undergo dramatic surface chemistry changes that may affect the interpretation of cellular uptake and cargo release data. On the other hand, it provides a rational explanation as to how ZIF-8 neatly dissolves in vivo.
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