The leucine zipper region of Myb oncoprotein regulates the commitment of hematopoietic progenitors

Author:

Karafiát Vı́t1,Dvořáková Marta1,Pajer Petr1,Králová Jarmila1,Hořejšı́ Zuzana1,Čermák Vladimı́r1,Bartůněk Petr1,Zenke Martin1,Dvořák Michal1

Affiliation:

1. From the Institute of Molecular Genetics, Academy of Sciences of the Czech Republic, Prague, and the Max-Delbrück Center for Molecular Medicine, Berlin, Germany.

Abstract

AbstractThe development of blood cells proceeds from pluripotent stem cells through multipotent progenitors into mature elements belonging to at least 8 different lineages. The lineage choice process during which stem cells and progenitors commit to a particular lineage is regulated by a coordinated action of extracellular signals and transcription factors. Molecular mechanisms controlling commitment are largely unknown. Here, the transcription factor v-Myb and its leucine zipper region (LZR) are identified as regulators of the commitment of a common myeloid progenitor and progenitors restricted to the myeloid lineage. It is demonstrated that wild-type v-Myb with the intact LZR directs development of progenitors into the macrophage lineage. Mutations in this region compromise commitment toward myeloid cells and cause v-Myb to also support the development of erythroid cells, thrombocytes, and granulocytes, similar to the c-Myb protein. In agreement with that, the wild-type v-Myb induces high expression of myeloid factors C/EBPβ, PU.1, and Egr-1 in its target cells, whereas SCL, GATA-1, and c-Myb are more abundant in cells expressing the v-Myb LZR mutant. It is proposed that Myb LZR can function as a molecular switch, affecting expression of lineage-specifying transcription factors and directing the development of hematopoietic progenitors into either myeloid or erythroid lineages.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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