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Synthesis and characterization of alginate/poly-L-ornithine/alginate microcapsules for local immunosuppression

机译:用于局部免疫抑制的藻酸盐/聚-L-鸟氨酸/藻酸盐微胶囊的合成与表征

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Alginate/poly-L-ornithine/alginate (APA) coherent microencapsulation, which provides an immunoselective and highly biocompatible membrane, creates a viable option for cellular or tissue transplantation. This study explored the potential of incorporating immunosuppressive drugs onto the capsule surface to provide local immunosuppression in addition to immunoisolation. A thorough investigation has been conducted to optimize and characterize alginate biotinylation via carbodiimide chemistry by a 4'-hydroxyazobenzene-2-carboxylic acid (HABA) based assay and by ATR-FTIR, H-NMR and XPS. To minimize the formation of by-product, a theoretical 40% activation of the carboxylic group on the alginate was employed to manufacture an optimal modification of ~10% biotinylated alginate. Confocal fluorescence microscopy was used to assess the conjugation of streptavidin and assembly of antibodies on the microcapsules. Local immunosuppressive capacity was assimilated on the APA microcapsules by binding of anti-tumour necrosis factor-alpha (TNF-α) antibodies via streptavidin-biotin conjugation, shown from the clear reduction of TNF-α in in-vitro medium.
机译:海藻酸盐/聚-L-鸟氨酸/海藻酸盐(APA)相干微囊封装可提供免疫选择性和高度生物相容性的膜,为细胞或组织移植创造了可行的选择。这项研究探索了将免疫抑制药物掺入胶囊表面以提供局部免疫抑制以及免疫隔离的潜力。通过基于碳二亚胺的化学反应,通过基于4'-羟基偶氮苯-2-羧酸(HABA)的测定以及ATR-FTIR,H-NMR和XPS,进行了彻底的研究以优化和表征藻酸盐生物素化。为了最大程度地减少副产物的生成,理论上将藻酸盐上羧基的40%活化用于制造〜10%生物素化藻酸盐的最佳修饰。共聚焦荧光显微镜用于评估抗生蛋白链菌素的缀合和微胶囊上抗体的组装。通过体外抗生物素蛋白-生物素的结合,抗肿瘤坏死因子-α(TNF-α)抗体的结合可以使APA微胶囊的局部免疫抑制能力得到同化,这从体外培养基中TNF-α的明显减少可以看出。

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