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冷冻系统及冷冻干燥过程中的相变:利用同步加速器X射线衍射法进行定量分析

Phase transitions in frozen systems and during freeze-drying: quantification using synchrotron X-ray diffractometry.

作者信息

Varshney Dushyant B, Sundaramurthi Prakash, Kumar Satyendra, Shalaev Evgenyi Y, Kang Shin-Woong, Gatlin Larry A, Suryanarayanan Raj

机构信息

Department of Pharmaceutics, College of Pharmacy, University of Minnesota, Minneapolis, Minnesota 55455, USA.

出版信息

Pharm Res. 2009 Jul;26(7):1596-606. doi: 10.1007/s11095-009-9868-4. Epub 2009 Mar 27.

Abstract

PURPOSE

(1) To develop a synchrotron X-ray diffraction (SXRD) method to monitor phase transitions during the entire freeze-drying cycle. Aqueous sodium phosphate buffered glycine solutions with initial glycine to buffer molar ratios of 1:3 (17:50 mM), 1:1 (50 mM) and 3:1 were utilized as model systems. (2) To investigate the effect of initial solute concentration on the crystallization of glycine and phosphate buffer salt during lyophilization.

METHODS

Phosphate buffered glycine solutions were placed in a custom-designed sample cell for freeze-drying. The sample cell, covered with a stainless steel dome with a beryllium window, was placed on a stage capable of controlled cooling and vacuum drying. The samples were cooled to -50 degrees C and annealed at -20 degrees C. They underwent primary drying at -25 degrees C under vacuum until ice sublimation was complete and secondary drying from 0 to 25 degrees C. At different stages of the freeze-drying cycle, the samples were periodically exposed to synchrotron X-ray radiation. An image plate detector was used to obtain time-resolved two-dimensional SXRD patterns. The ice, beta-glycine and DHPD phases were identified based on their unique X-ray peaks.

RESULTS

When the solutions were cooled and annealed, ice formation was followed by crystallization of disodium hydrogen phosphate dodecahydrate (DHPD). In the primary drying stage, a significant increase in DHPD crystallization followed by incomplete dehydration to amorphous disodium hydrogen phosphate was evident. Complete dehydration of DHPD occurred during secondary drying. Glycine crystallization was inhibited throughout freeze-drying when the initial buffer concentration (1:3 glycine to buffer) was higher than that of glycine.

CONCLUSION

A high-intensity X-ray diffraction method was developed to monitor the phase transitions during the entire freeze-drying cycle. The high sensitivity of SXRD allowed us to monitor all the crystalline phases simultaneously. While DHPD crystallizes in frozen solution, it dehydrates incompletely during primary drying and completely during secondary drying. The impact of initial solute concentration on the phase composition during the entire freeze-drying cycle was quantified.

摘要

目的

(1)开发一种同步加速器X射线衍射(SXRD)方法,以监测整个冷冻干燥循环中的相变。使用初始甘氨酸与缓冲剂摩尔比为1:3(17:50 mM)、1:1(50 mM)和3:1的磷酸钠缓冲甘氨酸水溶液作为模型系统。(2)研究初始溶质浓度对冷冻干燥过程中甘氨酸和磷酸盐缓冲盐结晶的影响。

方法

将磷酸盐缓冲甘氨酸溶液置于定制设计的样品池中进行冷冻干燥。样品池覆盖有带铍窗的不锈钢圆顶,放置在能够控制冷却和真空干燥的平台上。将样品冷却至-50℃并在-20℃下退火。它们在-25℃真空下进行一次干燥,直到冰升华完全,然后在0至25℃下进行二次干燥。在冷冻干燥循环的不同阶段,定期将样品暴露于同步加速器X射线辐射下。使用成像板探测器获取时间分辨二维SXRD图谱。根据其独特的X射线峰识别冰、β-甘氨酸和DHPD相。

结果

当溶液冷却和退火时,先形成冰,随后是十二水合磷酸氢二钠(DHPD)结晶。在一次干燥阶段,DHPD结晶显著增加,随后不完全脱水成无定形磷酸氢二钠。DHPD在二次干燥过程中完全脱水。当初始缓冲剂浓度(甘氨酸与缓冲剂之比为1:3)高于甘氨酸浓度时,整个冷冻干燥过程中甘氨酸结晶受到抑制。

结论

开发了一种高强度X射线衍射方法来监测整个冷冻干燥循环中的相变。SXRD的高灵敏度使我们能够同时监测所有晶相。虽然DHPD在冷冻溶液中结晶,但它在一次干燥过程中不完全脱水,在二次干燥过程中完全脱水。量化了初始溶质浓度对整个冷冻干燥循环中相组成的影响。

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