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Department of Biology Indiana University-Purdue University Indianapolis Indianapolis, Indiana 46202-5132
Lhx3 is a LIM homeodomain transcription factor
essential for pituitary development and motor neuron specification in
mice. We identified two isoforms of human Lhx3, hLhx3a and hLhx3b,
which differ in their ability to trans-activate pituitary
gene targets. These factors are identical within the LIM domains and
the homeodomain, but differ in their amino-terminal sequences preceding
the LIM motifs. Both isoforms are localized to the nucleus and are
expressed in the adult human pituitary, but gene activation studies
demonstrate characteristic functional differences. Human Lhx3a
trans-activated the
-glycoprotein subunit
promoter and a reporter construct containing a high-affinity Lhx3
binding site more effectively than the hLhx3b isoform. In addition,
hLhx3a synergized with the pituitary POU domain factor, Pit-1, to
strongly induce transcription of the
TSHß-subunit gene, while hLhx3b did not. We
demonstrate that the differences in gene activation properties between
hLhx3a and hLhx3b correlate with their DNA binding to sites within
these genes. The short hLhx3b-specific amino-terminal domain inhibits
DNA binding and gene activation functions of the molecule. These data
suggest that isoforms of Lhx3 may play distinct roles during
development of the mammalian pituitary gland and other neuroendocrine
systems.
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