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Molecular and Cellular Biology, April 1999, p. 2734-2745, Vol. 19, No. 4
0270-7306/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
COUP-TF Upregulates NGFI-A Gene
Expression through an Sp1 Binding Site
Carlos
Pipaón,
Sophia Y.
Tsai, and
Ming-Jer
Tsai*
Department of Cell Biology, Baylor College of
Medicine, Houston, Texas 77030
Received 19 October 1998/Returned for modification 24 November
1998/Accepted 11 January 1999
The formation of various tissues requires close communication
between two groups of cells, epithelial and mesenchymal cells. COUP-TFs
are transcription factors which have been shown to have functions in
embryonic development. COUP-TFI is expressed mainly in the nervous
system, and its targeted deletion leads to defects in the central and
peripheral nervous systems. COUP-TFII is highly expressed in the
mesenchymal component of the developing organs. A null mutation of
COUP-TFII results in the malformation of the heart and blood vessels.
From their expression pattern, we proposed that COUP-TFs regulate
paracrine signals important for mesenchymal cell-epithelial cell
interactions. In order to identify genes regulated by COUP-TF in this
process, a rat urogenital mesenchymal cell line was stably transfected
with a COUP-TFI expression vector. We found that NGFI-A, a
gene with important functions in brain, organ, and vasculature
development, has elevated mRNA and protein levels upon overexpression
of COUP-TFI in these cells. A study of the promoter region of this gene
identified a COUP-TF-responsive element between positions
64 and
46. Surprisingly, this region includes binding sites for members of
the Sp1 family of transcription factors but no COUP-TF binding site.
Mutations that abolish the Sp1 binding activity also impair the
transactivation of the NGFI-A promoter by COUP-TF. Two
regions of the COUP-TF molecule are shown to be important for
NGFI-A activation: the DNA binding domain and the extreme C
terminus of the putative ligand binding domain. The C-terminal region
is likely to be important for interaction with coactivators. In fact,
the coactivators p300 and steroid receptor activator 1 can enhance the
transactivation of the NGFI-A promoter induced by COUP-TFI.
Finally, we demonstrated that COUP-TF can directly interact with Sp1.
Taken together, these results suggest that NGFI-A is a
target gene for COUP-TFs and that the Sp1 family of transcription
factors mediates its regulation by COUP-TFs.
*
Corresponding author. Mailing address: Department of
Cell Biology, Baylor College of Medicine, One Baylor Plaza, Houston, TX
77030. Phone: (713) 798-6253. Fax: (713) 798-8227. E-mail: mtsai{at}bcm.tmc.edu.
Molecular and Cellular Biology, April 1999, p. 2734-2745, Vol. 19, No. 4
0270-7306/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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