类有机物
细胞生物学
胚胎干细胞
材料科学
生物
小岛
干细胞
组织工程
纳米技术
生物医学工程
医学
生物技术
基因
生物化学
胰岛素
作者
Joseph Candiello,Taraka Sai Pavan Grandhi,Saik Kia Goh,Vimal Vaidya,Maya Lemmon-Kishi,Kiarash Rahmani Eliato,Robert Ros,Prashant N. Kumta,Kaushal Rege,Ipsita Banerjee
出处
期刊:Biomaterials
[Elsevier]
日期:2018-05-25
卷期号:177: 27-39
被引量:139
标识
DOI:10.1016/j.biomaterials.2018.05.031
摘要
Organoids, which exhibit spontaneous organ specific organization, function, and multi-cellular complexity, are in essence the in vitro reproduction of specific in vivo organ systems. Recent work has demonstrated human pluripotent stem cells (hPSCs) as a viable regenerative cell source for tissue-specific organoid engineering. This is especially relevant for engineering islet organoids, due to the recent advances in generating functional beta-like cells from human pluripotent stem cells. In this study, we report specific engineering of regenerative islet organoids of precise size and cellular heterogeneity, using a novel hydrogel system, Amikagel. Amikagel facilitated controlled and spontaneous aggregation of human embryonic stem cell derived pancreatic progenitor cells (hESC-PP) into robust homogeneous spheroids. This platform further allowed fine control over the integration of multiple cell populations to produce heterogeneous spheroids, which is a necessity for complex organoid engineering. Amikagel induced hESC-PP spheroid formation enhanced pancreatic islet-specific Pdx-1 and NKX6.1 gene and protein expression, while also increasing the percentage of committed population. hESC-PP spheroids were further induced towards mature beta-like cells which demonstrated increased Beta-cell specific INS1 gene and C-peptide protein expression along with functional insulin production in response to in vitro glucose challenge. Further integration of hESC-PP with biologically relevant supporting endothelial cells resulted in multicellular organoids which demonstrated spontaneous maturation towards islet-specific INS1 gene and C-peptide protein expression along with a significantly developed extracellular matrix support system. These findings establish Amikagel –facilitated platform ideal for islet organoid engineering.
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