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猪胰岛封装于由甲基丙烯酸化壳聚糖二醇和海藻酸盐组成的免疫保护胶囊内。

Encapsulation of porcine pancreatic islets within an immunoprotective capsule comprising methacrylated glycol chitosan and alginate.

作者信息

Hillberg Anna Louise, Oudshoorn Matthew, Lam Janice B B, Kathirgamanathan Kalyani

机构信息

Living Cell Technologies (LCT), Auckland, New Zealand.

出版信息

J Biomed Mater Res B Appl Biomater. 2015 Apr;103(3):503-18. doi: 10.1002/jbm.b.33185. Epub 2014 Jun 11.

Abstract

Encapsulation of cells in biocompatible polymer matrices represents a powerful tool for cell-based therapies and therapeutic delivery systems. This technology has successfully been used to deliver pancreatic islets to humans for the treatment of Type 1 diabetes. However, the clinical impact of this technology may be improved by reducing the inflammatory response brought on after implantation of capsules in vivo. Within this study a biocompatible polymeric delivery system combining alginate and photo-crosslinked methacrylated glycol chitosan (MGC) was developed. This approach involved encapsulating cells in calcium-alginate beads, coating with MGC and photo-polymerizing using UVA in the presence of photo-initiator (VA-086), resulting in the formation of capsules ∼600 µm in size. Crosslinking of the MGC outer wall allowed control over capsule swelling and improved the capsules overall properties. Capsule characterization demonstrated the stabilizing influence of polymerization and fluorescence imaging showed that the distribution of glycol chitosan is dependent on molecular weight. Good islet viability and insulin release was demonstrated in vitro over the course of a month, and in vivo transplantation of the capsules demonstrated good biocompatibility, particularly when compared with standard alginate/poly-l-ornithine/alginate capsules.

摘要

将细胞封装在生物相容性聚合物基质中是基于细胞的治疗和治疗递送系统的有力工具。这项技术已成功用于将胰岛输送给人类以治疗1型糖尿病。然而,通过减少体内植入胶囊后引发的炎症反应,这项技术的临床效果可能会得到改善。在本研究中,开发了一种结合藻酸盐和光交联甲基丙烯酸化壳聚糖(MGC)的生物相容性聚合物递送系统。该方法包括将细胞封装在海藻酸钙珠中,用MGC包被,并在光引发剂(VA-086)存在下使用紫外线A进行光聚合,从而形成尺寸约为600 µm的胶囊。MGC外壁的交联可以控制胶囊的膨胀,并改善胶囊的整体性能。胶囊表征显示了聚合的稳定作用,荧光成像表明壳聚糖的分布取决于分子量。在体外一个月的时间里,胰岛显示出良好的活力和胰岛素释放,并且胶囊的体内移植显示出良好的生物相容性,特别是与标准藻酸盐/聚-L-鸟氨酸/藻酸盐胶囊相比。

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