PU. 1 determines the self-renewal capacity of erythroid progenitor cells

J Back, A Dierich, C Bronn, P Kastner, S Chan - Blood, 2004 - ashpublications.org
J Back, A Dierich, C Bronn, P Kastner, S Chan
Blood, 2004ashpublications.org
PU. 1 is a hematopoietic-specific transcriptional activator that is absolutely required for the
differentiation of B lymphocytes and myeloid-lineage cells. Although PU. 1 is also expressed
by early erythroid progenitor cells, its role in erythropoiesis, if any, is unknown. To
investigate the relevance of PU. 1 in erythropoiesis, we produced a line of PU. 1-deficient
mice carrying a green fluorescent protein reporter at this locus. We report here that PU. 1 is
tightly regulated during differentiation—it is expressed at low levels in erythroid progenitor …
Abstract
PU.1 is a hematopoietic-specific transcriptional activator that is absolutely required for the differentiation of B lymphocytes and myeloid-lineage cells. Although PU.1 is also expressed by early erythroid progenitor cells, its role in erythropoiesis, if any, is unknown. To investigate the relevance of PU.1 in erythropoiesis, we produced a line of PU.1-deficient mice carrying a green fluorescent protein reporter at this locus. We report here that PU.1 is tightly regulated during differentiation—it is expressed at low levels in erythroid progenitor cells and down-regulated upon terminal differentiation. Strikingly, PU.1-deficient fetal erythroid progenitors lose their self-renewal capacity and undergo proliferation arrest, premature differentiation, and apoptosis. In adult mice lacking one PU.1 allele, similar defects are detected following stress-induced erythropoiesis. These studies identify PU.1 as a novel and critical regulator of erythropoiesis and highlight the versatility of this transcription factor in promoting or preventing differentiation depending on the hematopoietic lineage.
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