Journal article

Repression of Flt3 by Pax5 is crucial for B-cell lineage commitment

ML Holmes, S Carotta, LM Corcoran, SL Nutt

Genes and Development | Published : 2006

DOI: 10.1101/gad.1396206

Abstract

Early B-lymphopoiesis requires the growth-factor receptors, IL-7R and Flt3, and the activity of a number of transcription factors. One factor, Pax5, is required for commitment to the B-cell lineage, although the molecular mechanism by which this occurs is unknown. We demonstrate here that an important function of Pax5 is to repress Flt3 transcription in B-cell progenitors, as Pax5-deficient pro-B cells express abundant Flt3 that is rapidly silenced upon the reintroduction of Pax5, whereas enforced expression of Flt3 in wild-type progenitors significantly impairs B-cell development. These findings demonstrate that the repression of Flt3 by Pax5 is essential for normal B-lymphopoiesis. © 2006 ..

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Keywords

Ligand
3101 Biochemistry and Cell Biology
Pax5
Stem-Cells
31 Biological Sciences
Flt3
Developmental Biology
Interleukin-7
Life Sciences & Biomedicine
Cancer
Hematopoietic Progenitor
Dendritic Cells
Genetics & Heredity
B-Cell Commitment
Transcriptional Repression
Stem Cell Research - Nonembryonic - Non-Human
Differentiation
Pro-B Cell
Identification
Science & Technology
Cell Biology
Bone-Marrow
Genetics
Generic Health Relevance
Stem Cell Research
C-Kit