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一种基于盐的方法来调节多孔胶原支架的刚度和生物降解性。

A salt-based method to adapt stiffness and biodegradability of porous collagen scaffolds.

作者信息

Versteegden Luuk R, Sloff Marije, Hoogenkamp Henk R, Pot Michiel W, Pang Jeffrey, Hafmans Theo G, de Jong Thijs, Smit Theo H, Leeuwenburgh Sander C, Oosterwijk Egbert, Feitz Wout F, Daamen Willeke F, van Kuppevelt Toin H

机构信息

Department of Biochemistry, Route 280, Radboud Institute for Molecular Life Sciences, Radboud university medical center P. O. Box 9101 6500 HB Nijmegen The Netherlands

Department of Urology, Route 267, Radboud Institute for Molecular Life Sciences, Radboud university medical center P. O. Box 9101 6500 HB Nijmegen The Netherlands.

出版信息

RSC Adv. 2019 Nov 12;9(63):36742-36750. doi: 10.1039/c9ra06651a. eCollection 2019 Nov 11.

Abstract

Type I collagen scaffolds for tissue reconstruction often have impaired mechanical characteristics such as limited stiffness and lack of strength. In this study, a new technique is presented to fine-tune stiffness and biodegradability of collagen scaffolds by treatment with concentrated salt solutions. Collagen scaffolds were prepared by a casting, freezing and lyophilization process. Scaffolds were treated with 90% saturated salt solutions, the salts taken from the Hofmeister series, followed by chemical crosslinking. Treatment with salts consisting of a divalent cation in combination with a monovalent anion, CaCl, resulted in fast shrinkage of the scaffolds up to approximately 10% of the original surface area. Effective salts were mostly at the chaotropic end of the Hofmeister series. Shrunken scaffolds were more than 10 times stiffer than non-shrunken control scaffolds, and displayed reduced pore sizes and swollen, less organized collagen fibrils. The effect could be pinpointed to the level of individual collagen molecules and indicates the shrinking effect to be driven by disruption of stabilizing hydrogen bonds within the triple helix. No calcium deposits remained in CaCl treated scaffolds. Subcutaneous implantation in rats showed similar biocompatibility compared to HO and NaCl treated scaffolds, but reduced cellular influx and increased structural integrity without signs of major degradation after 3 months. In conclusion, high concentrations of chaotropic salts can be used to adjust the mechanical characteristics of collagen scaffolds without affecting biocompatibility. This technique may be used in regenerative medicine to stiffen collagen scaffolds to better comply with the surrounding tissues, but may also be applied for slow release drug delivery systems.

摘要

用于组织重建的I型胶原支架通常具有机械性能受损的问题,如刚度有限和强度不足。在本研究中,提出了一种新技术,通过用浓盐溶液处理来微调胶原支架的刚度和生物降解性。胶原支架通过浇铸、冷冻和冻干工艺制备。支架用90%饱和盐溶液处理,这些盐取自霍夫迈斯特序列,然后进行化学交联。用由二价阳离子与一价阴离子组成的盐(CaCl)处理导致支架快速收缩,收缩至原始表面积的约10%。有效盐大多位于霍夫迈斯特序列的离液序列端。收缩后的支架比未收缩的对照支架硬10倍以上,且孔径减小,胶原纤维肿胀且排列不那么整齐。这种效应可以追溯到单个胶原分子水平,表明收缩效应是由三螺旋内稳定氢键的破坏驱动的。在CaCl处理的支架中没有残留钙沉积物。大鼠皮下植入显示与HO和NaCl处理的支架相比具有相似的生物相容性,但细胞流入减少,结构完整性增加,3个月后没有明显降解迹象。总之,高浓度的离液盐可用于调节胶原支架的机械性能而不影响生物相容性。该技术可用于再生医学中使胶原支架变硬以更好地顺应周围组织,也可应用于缓释药物递送系统。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a345/9075161/acde3e405662/c9ra06651a-f1.jpg

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