Human embryonic stem cells differentiate spontaneously in vitro into a range of cell types, and they frequently give rise to cells with the properties of extra-embryonic endoderm. We show here that endogenous signaling by bone morphogenetic protein-2 controls the differentiation of embryonic stem cells into this lineage. Treatment of embryonic stem cell cultures with the bone morphogenetic protein antagonist noggin blocks this form of differentiation and induces the appearance of a novel cell type that can give rise to neural precursors. These findings indicate that bone morphogenetic protein-2 controls a key early commitment step in human embryonic stem cell differentiation, and show that the conservation of developmental mechanisms at the cellular level can be exploited in this system – in this case, to provide a facile route for the generation of neural precursors from pluripotent cells.
Regulation of human embryonic stem cell differentiation by BMP-2 and its antagonist noggin
Present address: Hadassah University Hospital, 91120 Jerusalem, Israel
Martin F. Pera, Jessica Andrade, Souheir Houssami, Benjamin Reubinoff, Alan Trounson, Edouard G. Stanley, Dorien Ward-van Oostwaard, Christine Mummery; Regulation of human embryonic stem cell differentiation by BMP-2 and its antagonist noggin. J Cell Sci 1 March 2004; 117 (7): 1269–1280. doi: https://doi.org/10.1242/jcs.00970
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