Stage-specific signaling through TGFβ family members and WNT regulates patterning and pancreatic specification of human pluripotent stem cells

MC Nostro, F Sarangi, S Ogawa, A Holtzinger… - …, 2011 - journals.biologists.com
MC Nostro, F Sarangi, S Ogawa, A Holtzinger, B Corneo, X Li, SJ Micallef, IH Park
Development, 2011journals.biologists.com
The generation of insulin-producing β-cells from human pluripotent stem cells is dependent
on efficient endoderm induction and appropriate patterning and specification of this germ
layer to a pancreatic fate. In this study, we elucidated the temporal requirements for TGFβ
family members and canonical WNT signaling at these developmental stages and show that
the duration of nodal/activin A signaling plays a pivotal role in establishing an appropriate
definitive endoderm population for specification to the pancreatic lineage. WNT signaling …
The generation of insulin-producing β-cells from human pluripotent stem cells is dependent on efficient endoderm induction and appropriate patterning and specification of this germ layer to a pancreatic fate. In this study, we elucidated the temporal requirements for TGFβ family members and canonical WNT signaling at these developmental stages and show that the duration of nodal/activin A signaling plays a pivotal role in establishing an appropriate definitive endoderm population for specification to the pancreatic lineage. WNT signaling was found to induce a posterior endoderm fate and at optimal concentrations enhanced the development of pancreatic lineage cells. Inhibition of the BMP signaling pathway at specific stages was essential for the generation of insulin-expressing cells and the extent of BMP inhibition required varied widely among the cell lines tested. Optimal stage-specific manipulation of these pathways resulted in a striking 250-fold increase in the levels of insulin expression and yielded populations containing up to 25% C-peptide+ cells.
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