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基于壳聚糖/α,β-甘油磷酸盐冻干物的稳定热敏原位凝胶形成系统。

Stable thermosensitive in situ gel-forming systems based on the lyophilizate of chitosan/α,β-glycerophosphate salts.

作者信息

Wu Guanghao, Yuan Yuan, He Jintian, Li Ying, Dai Xiaojing, Zhao Baohua

机构信息

College of Life Science, Hebei Normal University, No. 20 Road East of 2nd Ring South, Shijiazhuang City, Hebei Province 050024, People's Republic of China.

College of Life Science, Hebei Normal University, No. 20 Road East of 2nd Ring South, Shijiazhuang City, Hebei Province 050024, People's Republic of China.

出版信息

Int J Pharm. 2016 Sep 10;511(1):560-569. doi: 10.1016/j.ijpharm.2016.07.050. Epub 2016 Jul 25.

DOI:10.1016/j.ijpharm.2016.07.050
PMID:27457422
Abstract

In the present study, lyophilization was attempted to improve the long-term storage of CS/GP thermogelling systems for biopharmaceutical applications. After lyophilization, CS/α,β-GP lyophilizate could not be dissolved in water, but some metal salts, such as NaCl, CaCl2, and MgCl2 surprisingly facilitated its dissolution. X-ray powder diffraction analysis suggested that calcium ions might preferentially form salts with α,β-GP, inhibit the transfer of protons from CS to α,β-GP, and then inhibit the aggregation of CS molecules during lyophilization. Comparison of the freshly prepared CS/α,β-GP/salt solutions and the reconstituted solutions from lyophilizates showed that lyophilization clearly influenced the properties of reconstituted CS/α,β-GP/salt solutions such as gelation time, viscosity, and pH. Furthermore, the reconstituted CS/α,β-GP/CaCl2 solutions maintained thermogelling properties and formed hydrogels at 37°C within approximately 5min, but did not form hydrogels at 20°C and 4°C over 2 weeks. The model protein bovine serum albumin (BSA) was further incorporated into the CS/α,β-GP/CaCl2 system. In vitro release experiments showed the sustained release of BSA from CS/α,β-GP/CaCl2 hydrogels in a pH-sensitive manner, demonstrating that CS/α,β-GP/CaCl2 may be useful as an in situ gel-forming system.

摘要

在本研究中,尝试采用冻干法来改善用于生物制药应用的CS/GP热凝胶系统的长期储存性能。冻干后,CS/α,β-GP冻干物不能溶解于水,但一些金属盐,如NaCl、CaCl2和MgCl2却出人意料地促进了其溶解。X射线粉末衍射分析表明,钙离子可能优先与α,β-GP形成盐,抑制质子从CS转移至α,β-GP,进而在冻干过程中抑制CS分子的聚集。将新制备的CS/α,β-GP/盐溶液与冻干物重构溶液进行比较,结果表明冻干明显影响了重构的CS/α,β-GP/盐溶液的性质,如凝胶化时间、粘度和pH值。此外,重构的CS/α,β-GP/CaCl2溶液保持了热凝胶性能,并在37°C下约5分钟内形成水凝胶,但在20°C和4°C下2周内未形成水凝胶。模型蛋白牛血清白蛋白(BSA)被进一步加入到CS/α,β-GP/CaCl2系统中。体外释放实验表明,BSA从CS/α,β-GP/CaCl2水凝胶中以pH敏感的方式持续释放,这表明CS/α,β-GP/CaCl2可能作为一种原位凝胶形成系统具有应用价值。

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