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Vol. 11, Issue 7, 2283-2295, July 2000
and
*Department of Biochemistry and Neuroscience Program, University of
Illinois, Urbana, Illinois 61801; and Previously, progesterone was found to regulate the initiation
and biosynthetic rate of myelin synthesis in Schwann cell/neuronal cocultures. The mRNA for cytochrome P450scc (converts cholesterol to
pregnenolone), 3
The Vanderbilt
Cancer Center, Department of Cell Biology, School of Medicine,
Vanderbilt University, Nashville, Tennessee 37232
-hydroxysteroid dehydrogenase (3
-HSD, converts pregnenolone to progesterone), and the progesterone receptor were found
to be markedly induced during active myelin synthesis. However, the
cells in the cocultures responsible for these changes were not
identified. In this study, in situ hybridization was used to determine
the localization of the enzymes responsible for steroid biosynthesis.
The mRNA for cytochrome P450scc and 3
-HSD were detected only in
actively myelinating cocultures and were localized exclusively in the
Schwann cells. Using immunocytochemistry, with minimal staining of the
Schwann cells, we found the progesterone receptor in the dorsal root
ganglia (DRG) neurons. The progesterone receptor in the neurons
translocated into the nuclei of these cells when progesterone was added
to neuronal cultures or during myelin synthesis in the cocultures.
Additionally, a marked induction of the progesterone receptor was found
in neuronal cultures after the addition of progesterone. The induction
of various genes in the neurons was also investigated using mRNA
differential display PCR in an attempt to elucidate the mechanism of
steroid action on myelin synthesis. Two novel genes were induced in
neuronal cultures by progesterone. These genes, along with the
progesterone receptor, were also induced in cocultures during myelin
synthesis, and their induction was blocked by RU-486 (a progesterone
receptor antagonist). These genes were not induced in Schwann cells
cultured alone after the addition of progesterone. These results
suggest that progesterone is synthesized in Schwann cells and that it can indirectly regulate myelin formation by activating transcription via the classical steroid receptor in the DRG neurons.
Corresponding author. E-mail address:
m-glaser{at}uiuc.edu.
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