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从胰岛移植中吸取的经验教训为基于干细胞的糖尿病治疗方法提供了启示。

Lessons from Human Islet Transplantation Inform Stem Cell-Based Approaches in the Treatment of Diabetes.

机构信息

The Barbara Davis Center for Diabetes, School of Medicine, University of Colorado Denver, Aurora, CO, United States.

Department of Pediatrics, School of Medicine, University of Minnesota, Minneapolis, MN, United States.

出版信息

Front Endocrinol (Lausanne). 2021 Mar 11;12:636824. doi: 10.3389/fendo.2021.636824. eCollection 2021.

Abstract

Diabetes mellitus is characterized by the body's inability to control blood glucose levels within a physiological range due to loss and/or dysfunction of insulin producing beta cells. Progressive beta cell loss leads to hyperglycemia and if untreated can lead to severe complications and/or death. Treatments at this time are limited to pharmacologic therapies, including exogenous insulin or oral/injectable agents that improve insulin sensitivity or augment endogenous insulin secretion. Cell transplantation can restore physiologic endogenous insulin production and minimize hyper- and hypoglycemic excursions. Islet isolation procedures and management of transplant recipients have advanced over the last several decades; both tight glycemic control and insulin independence are achievable. Research has been conducted in isolating islets, monitoring islet function, and mitigating the immune response. However, this procedure is still only performed in a small minority of patients. One major barrier is the scarcity of human pancreatic islet donors, variation in donor pancreas quality, and variability in islet isolation success. Advances have been made in generation of glucose responsive human stem cell derived beta cells (sBCs) and islets from human pluripotent stem cells using directed differentiation. This is an emerging promising treatment for patients with diabetes because they could potentially serve as an unlimited source of functional, glucose-responsive beta cells. Challenges exist in their generation including long term survival of grafts, safety of transplantation, and protection from the immune response. This review focuses on the progress made in islet allo- and auto transplantation and how these advances may be extrapolated to the sBC context.

摘要

糖尿病的特征是由于胰岛素产生β细胞的丧失和/或功能障碍,身体无法将血糖水平控制在生理范围内。β细胞的进行性丧失导致高血糖,如果不治疗,可能导致严重的并发症和/或死亡。目前的治疗方法仅限于药物治疗,包括外源性胰岛素或口服/注射剂,这些药物可以提高胰岛素敏感性或增强内源性胰岛素分泌。细胞移植可以恢复生理内源性胰岛素的产生,最大限度地减少高血糖和低血糖的波动。胰岛分离程序和移植受者的管理在过去几十年中得到了发展;既可以实现严格的血糖控制,也可以实现胰岛素独立性。已经进行了分离胰岛、监测胰岛功能和减轻免疫反应的研究。然而,这种手术目前仅在少数患者中进行。一个主要障碍是人类胰岛供体的稀缺性、供体胰腺质量的变化和胰岛分离成功率的变化。使用定向分化技术,从人类多能干细胞生成葡萄糖反应性人干细胞衍生β细胞(sBC)和胰岛方面已经取得了进展。这是一种有前途的糖尿病治疗方法,因为它们可能成为功能葡萄糖反应性β细胞的无限来源。其生成方面存在挑战,包括移植物的长期存活、移植的安全性以及免受免疫反应的保护。本文综述了胰岛同种异体和自体移植方面的进展,以及这些进展如何推广到 sBC 方面。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/99d0/7992005/8d699a7c9d2a/fendo-12-636824-g001.jpg

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