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Generation of pancreatic progenitors from human pluripotent stem cells by small molecules
Author(s) -
Yuqian Jiang,
Chuanxin Chen,
Lauren N. Randolph,
Songtao Ye,
Xin Zhang,
Xiaoping Bao,
Xiaojun Lian
Publication year - 2021
Publication title -
stem cell reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.207
H-Index - 76
ISSN - 2213-6711
DOI - 10.1016/j.stemcr.2021.07.021
Subject(s) - biology , wnt signaling pathway , microbiology and biotechnology , directed differentiation , induced pluripotent stem cell , cellular differentiation , progenitor cell , stem cell , transcriptome , foxa2 , embryonic stem cell , signal transduction , gene expression , genetics , gene
Human pluripotent stem cell (hPSC)-derived pancreatic progenitors (PPs) provide promising cell therapies for type 1 diabetes. Current PP differentiation requires a high amount of Activin A during the definitive endoderm (DE) stage, making it economically difficult for commercial ventures. Here we identify a dose-dependent role for Wnt signaling in controlling DE differentiation without Activin A. While high-level Wnt activation induces mesodermal formation, low-level Wnt activation by a small-molecule inhibitor of glycogen synthase kinase 3 is sufficient for DE differentiation, yielding SOX17 + FOXA2 + DE cells. BMP inhibition further enhances this DE differentiation, generating over 87% DE cells. These DE cells could be further differentiated into PPs and functional β cells. RNA-sequencing analysis of PP differentiation from hPSCs revealed expected transcriptome dynamics and new gene regulators during our small-molecule PP differentiation protocol. Overall, we established a robust growth-factor-free protocol for generating DE and PP cells, facilitating scalable production of pancreatic cells for regenerative applications.

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