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Islet-like organoids derived from human pluripotent stem cells efficiently function in the glucose responsiveness in vitro and in vivo

机译:源自人多能干细胞的胰岛样类器官在体外和体内均可有效发挥葡萄糖反应能力

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摘要

Insulin secretion is elaborately modulated in pancreatic ß cells within islets of three-dimensional (3D) structures. Using human pluripotent stem cells (hPSCs) to develop islet-like structures with insulin-producing ß cells for the treatment of diabetes is challenging. Here, we report that pancreatic islet-like clusters derived from hESCs are functionally capable of glucose-responsive insulin secretion as well as therapeutic effects. Pancreatic hormone-expressing endocrine cells (ECs) were differentiated from hESCs using a step-wise protocol. The hESC-derived ECs expressed pancreatic endocrine hormones, such as insulin, somatostatin, and pancreatic polypeptide. Notably, dissociated ECs autonomously aggregated to form islet-like, 3D structures of consistent sizes (100–150 μm in diameter). These EC clusters (ECCs) enhanced insulin secretion in response to glucose stimulus and potassium channel inhibition in vitro. Furthermore, ß cell-deficient mice transplanted with ECCs survived for more than 40 d while retaining a normal blood glucose level to some extent. The expression of pancreatic endocrine hormones was observed in tissues transplanted with ECCs. In addition, ECCs could be generated from human induced pluripotent stem cells. These results suggest that hPSC-derived, islet-like clusters may be alternative therapeutic cell sources for treating diabetes.
机译:胰岛β细胞在三维(3D)结构的胰岛中被精心调节。使用人类多能干细胞(hPSC)与产生胰岛素的ß细胞发展胰岛样结构来治疗糖尿病具有挑战性。在这里,我们报告从hESCs衍生的胰岛样群集功能上能够葡萄糖反应胰岛素的分泌以及治疗效果。胰腺激素表达的内分泌细胞(ECs)可以从人类胚胎干细胞中分步进行。来自hESC的EC表达胰腺内分泌激素,例如胰岛素,生长抑素和胰腺多肽。值得注意的是,解离的EC自主聚集形成大小一致(直径100-150μm)的胰岛状3D结构。这些EC簇(ECC)在体外响应葡萄糖刺激和钾通道抑制而增强了胰岛素分泌。此外,移植有ECC的ß细胞缺陷小鼠存活超过40 d,同时在一定程度上保持了正常的血糖水平。在移植了ECC的组织中观察到了胰腺内分泌激素的表达。另外,可以从人诱导的多能干细胞中产生ECC。这些结果表明,hPSC来源的胰岛样簇可能是治疗糖尿病的替代性治疗细胞来源。

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