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Molecular and Cellular Biology, October 1999, p. 7181-7190, Vol. 19, No. 10
0270-7306/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
C/EBP
Modulates the Early Events of Keratinocyte
Differentiation Involving Growth Arrest and Keratin 1 and Keratin
10 Expression
Songyun
Zhu,1
Hye-Sun
Oh,1,
Minsub
Shim,1
Esta
Sterneck,2,
Peter F.
Johnson,2 and
Robert
C.
Smart1,*
Molecular and Cellular Toxicology, Department
of Toxicology, North Carolina State University, Raleigh, North Carolina
27695-7633,1 and Eukaryotic
Transcriptional Regulation Group, ABL-Basic Research Program, National
Cancer Institute, Frederick Cancer Research and Development Center,
Frederick, Maryland 21702-12012
Received 10 February 1999/Returned for modification 19 March
1999/Accepted 30 June 1999
The epidermis is a stratified squamous epithelium composed
primarily of keratinocytes that become postmitotic and undergo sequential changes in gene expression during terminal differentiation. The expression of the transcription factor CCAAT/enhancer binding protein
(C/EBP
) within mouse epidermis and primary keratinocytes has recently been described; however, the function of C/EBP
within the epidermal keratinocyte is unknown. We report here that transient transfection of mouse primary keratinocytes with a C/EBP-responsive promoter-reporter construct resulted in a sevenfold increase in luciferase activity when keratinocytes were switched to culture conditions that induce growth arrest and differentiation. Forced expression of C/EBP
in BALB/MK2 keratinocytes inhibited growth, induced morphological changes consistent with a more differentiated phenotype, and upregulated two early markers of differentiation, keratin 1 (K1) and keratin 10 (K10) but had a minimal effect on the
expression of late-stage markers, loricrin and involucrin. Analysis of
the epidermis of C/EBP
-deficient mice revealed a mild epidermal
hyperplasia and decreased expression of K1 and K10 but not of
involucrin and loricrin. C/EBP
-deficient primary keratinocytes were
partially resistant to calcium-induced growth arrest. Analysis of
terminally differentiated spontaneously detached keratinocytes or those
induced to differentiate by suspension culture revealed that
C/EBP
-deficient keratinocytes displayed striking decreases in K1 and
K10, while expression of later-stage markers was only minimally
altered. Our results demonstrate that C/EBP
plays an important role
in the early events of stratified squamous differentiation in
keratinocytes involving growth arrest and K1 and K10 expression.
*
Corresponding author. Mailing address: Molecular and
Cellular Toxicology, Department of Toxicology, North Carolina State
University, Raleigh, NC 27695-7633. Phone: (919) 515-7245. Fax: (919)
515-7169. E-mail: rcsmart{at}unity.ncsu.edu.

Present address: Cutaneous Biology Research Center, Massachusetts
General Hospital, Harvard Medical School, Charlestown, MA
02115.

Present address: Molecular Mechanisms in Development Group, Basic
Research Laboratory, Division of Basic Sciences, National
Cancer
Institute, Frederick Cancer Research and Development Center,
Frederick,
MD 21702-1201.
Molecular and Cellular Biology, October 1999, p. 7181-7190, Vol. 19, No. 10
0270-7306/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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