高度聚乙烯糖基化的胰岛可在不使用免疫抑制药物的情况下改善同种异体胰岛移植的长期存活。

Dong Yun Lee, Sang Jin Park, Seulki Lee, Jong Hee Nam, Youngro Byun
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引用次数: 59

摘要

利用聚乙二醇(PEG)对胰岛进行表面修饰,作为防止宿主对移植胰岛产生免疫反应的一种手段,目前正在进行研究。在本研究中,为了用PEG分子完全保护胰岛,我们分别使用聚l -赖氨酸、聚烯丙胺或聚乙烯亚胺进行多次聚乙二醇化或扩增聚乙二醇化,从而增加了与胰岛表面结合的PEG的数量。扩增的聚乙二醇化与胰岛细胞毒性和功能损伤有关,但多次聚乙二醇化既不影响胰岛活力也不影响功能。此外,当三聚乙二醇化的胰岛移植到糖尿病受体中时,这些胰岛在没有任何免疫抑制治疗的情况下,在7名受体中有3名存活超过100天。此外,这3名患者的血糖水平稳定,在正常范围内。免疫组化分析显示,7例三聚乙二醇化胰岛移植中3例存活100 d, 4例在第20天前被排斥的胰岛移植均对免疫细胞具有免疫保护作用。然而,未经修饰的胰岛在1周内被完全破坏。因此,我们认为多重聚乙二醇化提供了一种有效的方法,通过增加表面结合的聚乙二醇的数量来降低移植胰岛的免疫原性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Highly poly(ethylene) glycolylated islets improve long-term islet allograft survival without immunosuppressive medication.

The surface modification of islets using poly(ethylene glycol) (PEG) is being studied as a means of preventing host immune responses against transplanted islets. In this study, to completely shield islets with PEG molecules, we increased the amount of PEG conjugated to islet surfaces, by multiple PEGylation or amplified PEGylation using poly-L-lysine, poly(allylamine), or poly(ethyleneimine), respectively. Amplified PEGylation was associated with islet cytotoxicity and functional impairment, but multiple PEGylation affected neither islet viability nor functionality. In addition, when triply PEGylated islets were allotransplanted into diabetic recipients, these islets survived in 3 of the 7 recipients for more than 100 days without any immunosuppressive treatment. Moreover, the blood glucose levels of these 3 recipients were stable and in the normal range. Immunohistochemical analysis showed that 3 of 7 triply PEGylated islets transplants survived for 100 days and that 4 that were rejected before day 20 were all immunologically protected from immune cells. However, unmodified islets were completely destroyed within 1 week. Consequently, we suggest that multiple PEGylation offers an effective means of reducing the immunogenicity of transplanted islets by increasing the amount of surface-bound PEG.

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来源期刊
Tissue engineering
Tissue engineering CELL & TISSUE ENGINEERING-BIOTECHNOLOGY & APPLIED MICROBIOLOGY
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