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Blood, Vol. 95 No. 8 (April 15), 2000:
pp. 2543-2551
GATA-1 interacts with the myeloid PU.1 transcription factor and
represses PU.1-dependent transcription
Claus Nerlov,
Erich Querfurth,
Holger Kulessa, and
Thomas Graf
From the Laboratory of Gene Therapy Research, Copenhagen University
Hospital Copenhagen, Denmark; the European Molecular Biology
Laboratory, Heidelberg, Germany; and the Albert Einstein College of
Medicine, Bronx, NY.
The GATA-1 transcription factor is capable of suppressing the
myeloid gene expression program when ectopically expressed in myeloid
cells. We examined the ability of GATA-1 to repress the expression and
function of the PU.1 transcription factor, a central regulator of
myeloid differentiation. We found that GATA-1 is capable of suppressing
the myeloid phenotype without interfering with PU.1 gene expression,
but instead was capable of inhibiting the activity of the PU.1 protein
in a dose-dependent manner. This inhibition was independent of the
ability of GATA-1 to bind DNA, suggesting that it is mediated by
protein-protein interaction. We examined the ability of PU.1 to
interact with GATA-1 and found a direct interaction between the PU.1
ETS domain and the C-terminal finger region of GATA-1. Replacing the
PU.1 ETS domain with the GAL4 DNA-binding domain removed the ability of
GATA-1 to inhibit PU.1 activity, indicating that the PU.1 DNA-binding
domain, rather than the transactivation domain, is the target for
GATA-1-mediated repression. We therefore propose that GATA-1 represses
myeloid gene expression, at least in part, through its ability to
directly interact with the PU.1 ETS domain and thereby interfere with
PU.1 function.

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Modulation of Endogenous GATA-4 Activity Reveals Its Dual Contribution to Mullerian Inhibiting Substance Gene Transcription in Sertoli Cells
Mol. Endocrinol.,
September 1, 2001;
15(9):
1636 - 1650.
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P. Zhang, X. Zhang, A. Iwama, C. Yu, K. A. Smith, B. U. Mueller, S. Narravula, B. E. Torbett, S. H. Orkin, and D. G. Tenen
PU.1 inhibits GATA-1 function and erythroid differentiation by blocking GATA-1 DNA binding
Blood,
October 15, 2000;
96(8):
2641 - 2648.
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E. Querfurth, M. Schuster, H. Kulessa, J. D. Crispino, G. Döderlein, S. H. Orkin, T. Graf, and C. Nerlov
Antagonism between C/EBPbeta and FOG in eosinophil lineage commitment of multipotent hematopoietic progenitors
Genes & Dev.,
October 1, 2000;
14(19):
2515 - 2525.
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I. Matsumura, A. Kawasaki, H. Tanaka, J. Sonoyama, S. Ezoe, N. Minegishi, K. Nakajima, M. Yamamoto, and Y. Kanakura
Biologic significance of GATA-1 activities in Ras-mediated megakaryocytic differentiation of hematopoietic cell lines
Blood,
October 1, 2000;
96(7):
2440 - 2450.
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X. Yu and S. M. Weissman
Characterization of the Promoter of Human Leukocyte-specific Transcript 1. A SMALL GENE WITH A COMPLEX PATTERN OF ALTERNATIVE TRANSCRIPTS
J. Biol. Chem.,
October 27, 2000;
275(44):
34597 - 34608.
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A. Verger, E. Buisine, S. Carrere, R. Wintjens, A. Flourens, J. Coll, D. Stehelin, and M. Duterque-Coquillaud
Identification of Amino Acid Residues in the ETS Transcription Factor Erg That Mediate Erg-Jun/Fos-DNA Ternary Complex Formation
J. Biol. Chem.,
May 11, 2001;
276(20):
17181 - 17189.
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J. Hernandez-Torres, M. Yunta, and P. A. Lazo
Differential Cooperation between Regulatory Sequences Required for Human CD53 Gene Expression
J. Biol. Chem.,
September 14, 2001;
276(38):
35405 - 35413.
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A. Newton, J. Mackay, and M. Crossley
The N-terminal Zinc Finger of the Erythroid Transcription Factor GATA-1 Binds GATC Motifs in DNA
J. Biol. Chem.,
September 14, 2001;
276(38):
35794 - 35801.
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