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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Embryonic pig pancreatic tissue for the treatment of diabetes: potential role of immune suppression with 'off-the-shelf' third-party regulatory T cells.
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Embryonic pig pancreatic tissue for the treatment of diabetes: potential role of immune suppression with 'off-the-shelf' third-party regulatory T cells.

机译:用于治疗糖尿病的猪胚胰腺组织:“现成的”第三方调节性T细胞对免疫抑制的潜在作用。

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BACKGROUND: Xenogeneic embryonic pancreatic tissue can provide an attractive alternative for organ replacement therapy. However, immunological rejection represents a major obstacle. This study examines the potential of regulatory T cells (Tregs) in the prevention of E42 pancreas rejection. METHODS: To develop new approaches to combat rejection, we evaluated engraftment, growth, and development of E42 pig pancreatic tissue in mice treated with ex vivo expanded Tregs in combination with T-cell debulking and the conventional immunosuppressive drugs, rapamycin and FTY720. RESULTS: Transplantation of E42 pig pancreas into C57BL/6 mice immunosuppressed by this protocol resulted in complete rejection within less than 6 weeks. In contrast, additional treatment with a single infusion of ex vivo expanded third-party Tregs markedly delayed the onset of graft rejection to 10 weeks. The infusion of Tregs was associated with a significant reduction in CD4 and CD8 expansion in the lymph nodes and other peripheral organs at the priming stages after implantation. Freezing and thawing of the Tregs did not affect their efficacy, indicating the potential of Tregs banking. CONCLUSION: Considering the technical difficulties encountered in the generation of Tregs from patients or from specific donors, our results demonstrate the feasibility of using "off-the-shelf" fresh or frozen third-party Tregs to control rejection in organ transplantation.
机译:背景:异种胚胎胰腺组织可以为器官替代治疗提供有吸引力的替代方法。但是,免疫排斥是主要障碍。这项研究检查了调节性T细胞(Tregs)在预防E42胰腺排斥中的潜力。方法:为开发抗排斥的新方法,我们评估了离体扩增Treg结合T细胞减灭和常规免疫抑制药物雷帕霉素和FTY720治疗的小鼠E42猪胰腺组织的植入,生长和发育。结果:该协议免疫抑制的E42猪胰腺移植到C57BL / 6小鼠中,导致在不到6周的时间内完全排斥。相比之下,单次注入体外扩增的第三方Treg进行的其他治疗将移植排斥反应的发生明显延迟了10周。 Tregs的注入与植入后启动阶段的淋巴结和其他周围器官的CD4和CD8扩增显着减少有关。 Tregs的冻结和解冻不影响其功效,表明Tregs银行业务的潜力。结论:考虑到从患者或特定供体产生Treg时遇到的技术困难,我们的结果证明了使用“现成”的新鲜或冷冻第三方Treg来控制器官移植排斥的可行性。

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