Figure 6
PcG proteins behave differentially in fetal liver and adult BM HSCs. In this study, Ezh1 contributed little to fetal liver HSCs similar to a PRC1 protein, Bmi1, even in the absence of Ezh2 (top left panel, wild-type HSCs; bottom left panel, Ezh2−/− HSCs). In BM, Ezh2-mediated gene silencing is reinforced by Ezh1 and mono-ubiquitylation at H2AK119 by Bmi1-containing PRC2 (top right panel, wild-type HSCs; bottom right panel, Ezh2−/− HSCs). Differential epigenetic regulation by PcG proteins might have a strong impact on the cell cycle status of proliferative fetal and quiescent adult HSCs.

PcG proteins behave differentially in fetal liver and adult BM HSCs. In this study, Ezh1 contributed little to fetal liver HSCs similar to a PRC1 protein, Bmi1, even in the absence of Ezh2 (top left panel, wild-type HSCs; bottom left panel, Ezh2−/− HSCs). In BM, Ezh2-mediated gene silencing is reinforced by Ezh1 and mono-ubiquitylation at H2AK119 by Bmi1-containing PRC2 (top right panel, wild-type HSCs; bottom right panel, Ezh2−/− HSCs). Differential epigenetic regulation by PcG proteins might have a strong impact on the cell cycle status of proliferative fetal and quiescent adult HSCs.

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