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Research Institute, Hospital for Sick Children, Departments
of Clinical Biochemistry and Biochemistry, University of Toronto
(D.L., Y.L.D., F.X., C.L.H.), Toronto, Ontario, Canada,
Loeb Institute for Medical Research, Ottawa Civic Hospital and
University of Ottawa (M.E.), Ottawa, Ontario, Canada
Steroidogenic factor 1, a member of the
fushi tarazu factor 1 (FTZ-F1) subfamily of nuclear
receptors, is a key regulator in mammalian reproduction. From an
embryonic complementary DNA library, the zebrafish homolog of FTZ-F1
(zFF1A) and an alternatively spliced variant (zFF1B) were isolated.
zFF1B represented a C-terminally truncated version of zFF1A. Whole
mount in situ hybridization and reverse transcriptase-PCR
analysis revealed that both zFF1A and B transcripts were present in the
developing pituitaries, adult fish brain, gonads, and liver, albeit
zFF1B messenger RNA was absent in testis. Comparison of the primary
sequences of zFF1 with those of other FTZ-F1 subfamily members showed a
close structural relationship between the mouse liver receptor homolog,
which activated the
1-fetoprotein gene in
rodent liver. However, similar to mouse steroidogenic factor 1, zFF1A
regulated chinook salmon gonadotropin IIß subunit gene expression. On
the contrary, zFF1B, which could bind a consensus gonadotrope-specific
element with an affinity similar to that of zFF1A, lacked both the
trans-activation function and synergistic interaction with
the estrogen receptor. Furthermore, cotransfection studies in HeLa
cells showed that zFF1B was a strong competitor for the action of zFF1A
on the chinook salmon gonadotropin IIß subunit gene promoter. Our
investigation suggests that 1) zFF1 represents an ancestor protein of
the vertebrate FTZ-F1 homologs; 2) the antagonistic relationship
between zFF1A and -B may dictate the expression of the FTZ-F1 target
genes in a variety of tissues, including the pituitary; and 3) the
naturally occurring zFF1B provides evidence that the C-terminal portion
of zFF1A (80 amino acid residues) contains a major
trans-activation function and a protein-protein interface.
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