Maturation stage–specific regulation of megakaryopoiesis by pointed-domain Ets proteins

Author:

Pang Liyan1,Xue Hai-Hui1,Szalai Gabor1,Wang Xun1,Wang Yuhuan1,Watson Dennis K.1,Leonard Warren J.1,Blobel Gerd A.1,Poncz Mortimer1

Affiliation:

1. From the Department of Pediatrics, Children's Hospital of Philadelphia and the University of Pennsylvania School of Medicine; the Laboratory of Molecular Immunology, National Heart, Lung, and Blood Institute, Bethesda, MD; the Departments of Pathology and Laboratory Medicine and Biochemistry and Molecular Biology, Hollings Cancer Center, Medical University of South Carolina, Charleston.

Abstract

AbstractNumerous megakaryocyte-specific genes contain signature Ets-binding sites in their regulatory regions. Fli-1 (friend leukemia integration 1), an Ets transcription factor, is required for the normal maturation of megakaryocytes and controls the expression of multiple megakaryocyte-specific genes. However, in Fli-1–/– mice, early megakaryopoiesis persists, and the expression of the early megakaryocyte-specific genes, αIIb and cMpl, is maintained, consistent with functional compensation by a related Ets factor(s). Here we identify the Ets protein GABPα (GA-binding protein α) as a regulator of early megakaryocyte-specific genes. Notably, GABPα preferentially occupies Ets elements of early megakaryocyte-specific genes in vitro and in vivo, whereas Fli-1 binds both early and late megakaryocyte-specific genes. Moreover, the ratio of GABPα/Fli-1 expression declines throughout megakaryocyte maturation. Consistent with this expression pattern, primary fetal liver–derived megakaryocytes from Fli-1–deficient murine embryos exhibit reduced expression of genes associated with late stages of maturation (glycoprotein [GP] Ibα, GPIX, and platelet factor 4 [PF4]), whereas GABPα-deficient megakaryocytes were mostly impaired in the expression of early megakaryocyte-specific genes (αIIb and cMpl). Finally, mechanistic experiments revealed that GABPα, like Fli-1, can impart transcriptional synergy between the hematopoietic transcription factor GATA-1 and its cofactor FOG-1 (friend of GATA-1). In concert, these data reveal disparate, but overlapping, functions of Ets transcription factors at distinct stages of megakaryocyte maturation.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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