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Co-culture with Mature Islet Cells Augments the Differentiation of Insulin-Producing Cells from Pluripotent Stem Cells

机译:与成熟胰岛细胞共培养可增强多能干细胞与胰岛素生产细胞的分化。

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Islet transplantation has been hampered by the shortage of islet donors available for diabetes therapy. However, pluripotent stem cells (PSCs) can be an alternative source of insulin-producing cells (IPCs) because of their capacity for self-renewal and differentiation. We described a method to efficiently differentiate PSCs into IPCs by co-culturing mature islets with directed-differentiated pancreatic endoderm (PE) cells from mouse and human PSCs. PE cells co-cultured with islet cells or islet cell-derived conditioned medium (CM) showed increased expression levels of beta-cell markers; significantly higher levels of proinsulin- and Newport Green (NG)-positive cells, which revealed the characteristics of insulin producing cells; and increased insulin secretion upon glucose stimulation. Co-culturing human PE cells with islet cells was also effective to differentiate PE cells into IPCs. Diabetic nude mice transplanted with co-cultured cells exhibited restored euglycemia, human C-peptide release, and improved glucose tolerance. Immunohistochemistry revealed that insulin+/C-peptide + cells existed in the grafted tissues. These results suggest that mature islet cells can increase the differentiation efficiency of PE cells into mature IPCs via paracrine effects.
机译:胰岛移植受到可用于糖尿病治疗的胰岛供体短缺的阻碍。但是,由于多能干细胞具有自我更新和分化的能力,因此它可以成为胰岛素生产细胞(IPC)的替代来源。我们描述了一种通过与小鼠和人类PSC的定向分化的胰腺内胚层(PE)细胞共培养成熟胰岛来有效地将PSC分化为IPC的方法。与胰岛细胞或胰岛细胞衍生的条件培养基(CM)共培养的PE细胞显示出增加的β细胞标记物表达水平;胰岛素原和新港绿(NG)阳性细胞的水平显着升高,这揭示了产生胰岛素的细胞的特征;并在葡萄糖刺激下增加胰岛素分泌。将人类PE细胞与胰岛细胞共同培养也可以有效地将PE细胞分化为IPC。移植有共培养细胞的糖尿病裸鼠表现出恢复的正常血糖,人C肽释放和改善的葡萄糖耐量。免疫组织化学显示,移植组织中存在胰岛素+ / C-肽+细胞。这些结果表明,成熟的胰岛细胞可以通过旁分泌作用提高PE细胞向成熟IPC分化的效率。

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