Differential regulation of Foxo3a target genes in erythropoiesis

Walbert J. Bakker; Thamar B. van Dijk; Martine Parren-van Amelsvoort; Andrea Kolbus; Kazuo Yamamoto; Peter Steinlein; Roel G. W. Verhaak; Tak W. Mak; Hartmut Beug; Bob Löwenberg; Marieke von Lindern

doi:10.1128/MCB.01662-06

Differential regulation of Foxo3a target genes in erythropoiesis

Walbert J. Bakker, Thamar B. van Dijk, Martine Parren-van Amelsvoort, Andrea Kolbus, Kazuo Yamamoto, Peter Steinlein, Roel G. W. Verhaak, Tak W. Mak, Hartmut Beug, Bob Löwenberg, Marieke von Lindern

Research output: Contribution to journal › Article › Academic › peer-review

67 Citations (Scopus)

Abstract

The cooperation of stem cell factor (SCF) and erythropoietin (Epo) is required to induce renewal divisions in erythroid progenitors, whereas differentiation to mature erythrocytes requires the presence of Epo only. Epo and SCF activate common signaling pathways such as the activation of protein kinase B (PKB) and the subsequent phosphorylation and inactivation of Foxo3a. In contrast, only Epo activates Stat5. Both Foxo3a and Stat5 promote erythroid differentiation. To understand the interplay of SCF and Epo in maintaining the balance between renewal and differentiation during erythroid development, we investigated differential Foxo3a target regulation by Epo and SCF. Expression profiling revealed that a subset of Foxo3a targets was not inhibited but was activated by Epo. One of these genes was Cited2. Transcriptional control of Epo/Foxo3a-induced Cited2 was studied and compared with that of the Epo-repressed Foxo3a target Btg1. We show that in response to Epo, the allegedly growth-inhibitory factor Foxo3a associates with the allegedly growth-stimulatory factor Stat5 in the nucleus, which is required for Epo-induced Cited2 expression. In contrast, Btg1 expression is controlled by the cooperation of Foxo3a with cyclic AMP- and Jun kinase-dependent Creb family members. Thus, Foxo3a not only is an effector of PKB but also integrates distinct signals to regulate gene expression in erythropoiesis

Original language	English
Pages (from-to)	3839-3854
Journal	Molecular and cellular biology
Volume	27
Issue number	10
DOIs	https://doi.org/10.1128/MCB.01662-06
Publication status	Published - 2007

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@article{391c9c5815a64c0a9ec75ee734162041,

title = "Differential regulation of Foxo3a target genes in erythropoiesis",

abstract = "The cooperation of stem cell factor (SCF) and erythropoietin (Epo) is required to induce renewal divisions in erythroid progenitors, whereas differentiation to mature erythrocytes requires the presence of Epo only. Epo and SCF activate common signaling pathways such as the activation of protein kinase B (PKB) and the subsequent phosphorylation and inactivation of Foxo3a. In contrast, only Epo activates Stat5. Both Foxo3a and Stat5 promote erythroid differentiation. To understand the interplay of SCF and Epo in maintaining the balance between renewal and differentiation during erythroid development, we investigated differential Foxo3a target regulation by Epo and SCF. Expression profiling revealed that a subset of Foxo3a targets was not inhibited but was activated by Epo. One of these genes was Cited2. Transcriptional control of Epo/Foxo3a-induced Cited2 was studied and compared with that of the Epo-repressed Foxo3a target Btg1. We show that in response to Epo, the allegedly growth-inhibitory factor Foxo3a associates with the allegedly growth-stimulatory factor Stat5 in the nucleus, which is required for Epo-induced Cited2 expression. In contrast, Btg1 expression is controlled by the cooperation of Foxo3a with cyclic AMP- and Jun kinase-dependent Creb family members. Thus, Foxo3a not only is an effector of PKB but also integrates distinct signals to regulate gene expression in erythropoiesis",

author = "Bakker, {Walbert J.} and {van Dijk}, {Thamar B.} and {Parren-van Amelsvoort}, Martine and Andrea Kolbus and Kazuo Yamamoto and Peter Steinlein and Verhaak, {Roel G. W.} and Mak, {Tak W.} and Hartmut Beug and Bob L{\"o}wenberg and {von Lindern}, Marieke",

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doi = "10.1128/MCB.01662-06",

language = "English",

volume = "27",

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journal = "Molecular and cellular biology",

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T1 - Differential regulation of Foxo3a target genes in erythropoiesis

AU - Bakker, Walbert J.

AU - van Dijk, Thamar B.

AU - Parren-van Amelsvoort, Martine

AU - Kolbus, Andrea

AU - Yamamoto, Kazuo

AU - Steinlein, Peter

AU - Verhaak, Roel G. W.

AU - Mak, Tak W.

AU - Beug, Hartmut

AU - Löwenberg, Bob

AU - von Lindern, Marieke

PY - 2007

Y1 - 2007

N2 - The cooperation of stem cell factor (SCF) and erythropoietin (Epo) is required to induce renewal divisions in erythroid progenitors, whereas differentiation to mature erythrocytes requires the presence of Epo only. Epo and SCF activate common signaling pathways such as the activation of protein kinase B (PKB) and the subsequent phosphorylation and inactivation of Foxo3a. In contrast, only Epo activates Stat5. Both Foxo3a and Stat5 promote erythroid differentiation. To understand the interplay of SCF and Epo in maintaining the balance between renewal and differentiation during erythroid development, we investigated differential Foxo3a target regulation by Epo and SCF. Expression profiling revealed that a subset of Foxo3a targets was not inhibited but was activated by Epo. One of these genes was Cited2. Transcriptional control of Epo/Foxo3a-induced Cited2 was studied and compared with that of the Epo-repressed Foxo3a target Btg1. We show that in response to Epo, the allegedly growth-inhibitory factor Foxo3a associates with the allegedly growth-stimulatory factor Stat5 in the nucleus, which is required for Epo-induced Cited2 expression. In contrast, Btg1 expression is controlled by the cooperation of Foxo3a with cyclic AMP- and Jun kinase-dependent Creb family members. Thus, Foxo3a not only is an effector of PKB but also integrates distinct signals to regulate gene expression in erythropoiesis

AB - The cooperation of stem cell factor (SCF) and erythropoietin (Epo) is required to induce renewal divisions in erythroid progenitors, whereas differentiation to mature erythrocytes requires the presence of Epo only. Epo and SCF activate common signaling pathways such as the activation of protein kinase B (PKB) and the subsequent phosphorylation and inactivation of Foxo3a. In contrast, only Epo activates Stat5. Both Foxo3a and Stat5 promote erythroid differentiation. To understand the interplay of SCF and Epo in maintaining the balance between renewal and differentiation during erythroid development, we investigated differential Foxo3a target regulation by Epo and SCF. Expression profiling revealed that a subset of Foxo3a targets was not inhibited but was activated by Epo. One of these genes was Cited2. Transcriptional control of Epo/Foxo3a-induced Cited2 was studied and compared with that of the Epo-repressed Foxo3a target Btg1. We show that in response to Epo, the allegedly growth-inhibitory factor Foxo3a associates with the allegedly growth-stimulatory factor Stat5 in the nucleus, which is required for Epo-induced Cited2 expression. In contrast, Btg1 expression is controlled by the cooperation of Foxo3a with cyclic AMP- and Jun kinase-dependent Creb family members. Thus, Foxo3a not only is an effector of PKB but also integrates distinct signals to regulate gene expression in erythropoiesis

U2 - 10.1128/MCB.01662-06

DO - 10.1128/MCB.01662-06

M3 - Article

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SN - 0270-7306

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JO - Molecular and cellular biology

JF - Molecular and cellular biology

IS - 10

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