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Novel freeze-drying methods to produce a range of collagen-glycosaminoglycan scaffolds with tailored mean pore sizes.

机译:新型冷冻干燥方法可生产一系列具有定制平均孔径的胶原蛋白-糖胺聚糖支架。

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摘要

The pore structure of three-dimensional scaffolds used in tissue engineering has been shown to significantly influence cellular activity. As the optimal pore size is dependant on the specifics of the tissue engineering application, the ability to alter the pore size over a wide range is essential for a particular scaffold to be suitable for multiple applications. With this in mind, the aim of this study was to develop methodologies to produce a range of collagen-glycosaminoglycan (CG) scaffolds with tailored mean pore sizes. The pore size of CG scaffolds is established during the freeze-drying fabrication process. In this study, freezing temperature was varied (−10 degrees C to −70 degrees C) and an annealing step was introduced to the process to determine their effects on pore size. Annealing is an additional step in the freeze-drying cycle that involves raising the temperature of the frozen suspension to increase the rate of ice crystal growth. The results show that the pore size of the scaffolds decreased as the freezing temperature was reduced. Additionally, the introduction of an annealing step during freeze-drying was found to result in a significant increase (40%) in pore size. Taken together, these results demonstrate that the methodologies developed in this study can be used to produce a range of CG scaffolds with mean pore sizes from 85 to 325 microm. This is a substantial improvement on the range of pore sizes that were possible to produce previously (96-150 microm). The methods developed in this study provide a basis for the investigation of the effects of pore size on both in vitro and in vivo performance and for the determination of the optimal pore structure for specific tissue engineering applications.
机译:已显示用于组织工程的三维支架的孔结构显着影响细胞活性。由于最佳孔径取决于组织工程应用的具体情况,因此在较大范围内改变孔径的能力对于特定支架适合多种应用至关重要。考虑到这一点,本研究的目的是开发一种方法,以生产一系列具有定制平均孔径的胶原蛋白-糖胺聚糖(CG)支架。 CG支架的孔径是在冷冻干燥过程中确定的。在这项研究中,改变了冷冻温度(-10℃至-70℃),并在该工艺中引入了退火步骤,以确定它们对孔径的影响。退火是冷冻干燥循环中的附加步骤,其涉及升高冷冻悬浮液的温度以增加冰晶的生长速率。结果表明,随着冷冻温度的降低,支架的孔径减小。另外,发现在冷冻干燥过程中引入退火步骤导致孔径显着增加(40%)。综上所述,这些结果表明,本研究中开发的方法可用于生产一系列平均孔径从85到325微米的CG支架。这是对以前可能产生的孔径范围(96-150微米)的重大改进。这项研究中开发的方法为研究孔径对体外和体内性能的影响以及确定针对特定组织工程应用的最佳孔结构提供了基础。

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