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Genetically Engineered Islets and Alternative Sources of Insulin-Producing Cells for Treating Autoimmune Diabetes: Quo Vadis?

机译:基因改造的胰岛和胰岛素产生细胞的替代来源用于治疗自身免疫性糖尿病:Qu Vadis吗?

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摘要

Islet transplantation is a promising therapy for patients with type 1 diabetes that can provide moment-to-moment metabolic control of glucose and allow them to achieve insulin independence. However, two major problems need to be overcome: (1) detrimental immune responses, including inflammation induced by the islet isolation/transplantation procedure, recurrence autoimmunity, and allorejection, can cause graft loss and (2) inadequate numbers of organ donors. Several gene therapy approaches and pharmaceutical treatments have been demonstrated to prolong the survival of pancreatic islet grafts in animal models; however, the clinical applications need to be investigated further. In addition, for an alternative source of pancreatic β-cell replacement therapy, the ex vivo generation of insulin-secreting cells from diverse origins of stem/progenitor cells has become an attractive option in regenerative medicine. This paper focuses on the genetic manipulation of islets during transplantation therapy and summarizes current strategies to obtain functional insulin-secreting cells from stem/progenitor cells.
机译:对于1型糖尿病患者,胰岛移植是一种有前途的疗法,可以提供瞬间对葡萄糖的新陈代谢控制,并使他们获得胰岛素独立性。但是,需要克服两个主要问题:(1)有害的免疫反应,包括由胰岛分离/移植过程引起的炎症,复发性自身免疫和同种异体注射,可能会导致移植物丢失,以及(2)器官供体数量不足。在动物模型中,已经证明了几种基因治疗方法和药物治疗可以延长胰岛移植物的存活。然而,临床应用需要进一步研究。另外,对于胰腺β细胞替代疗法的替代来源,来自干细胞/祖细胞的多种来源的胰岛素分泌细胞的离体产生已成为再生医学中的有吸引力的选择。本文着重于胰岛移植治疗过程中的基因操作,并总结了当前从干细胞/祖细胞获得功能性胰岛素分泌细胞的策略。

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