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Departments of Cell Biology and Physiology and Obstetrics, Gynecology and Reproductive Sciences (A.J.Z.) and Magee Womens Research Institute (D.F.B., A.J.Z.), University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15213
Address all correspondence and requests for reprints to: A. J. Zeleznik, Ph.D., Magee-Womens Research Institute, 204 Craft Avenue, Pittsburgh, Pennsylvania 15213.
Recent studies from our laboratory demonstrating that the expression of
cAMP-dependent nuclear transcription factor CREB (cAMP response element
binding protein) is lost following ovulation in macaques has revealed a
novel mechanism by which the cytoplasmic and nuclear actions the
cAMP-protein kinase A (PKA) intracellular signaling system may be
regulated independently. Implicit in this hypothesis is the assumption
that PKA activity is maintained throughout the luteal phase of the
menstrual cycle, yet to date there have been no published reports
regarding PKA activity in the primate corpus luteum. PKA activity was
assessed by the incorporation of 32P from radiolabeled ATP
into a PKA-specific peptide substrate (kemptide) in the presence or
absence of cAMP. Luteal cytosolic fractions were obtained from corpora
lutea collected during the spontaneous luteal phase (days 35, 78,
1011, 1315, and postmenses) or obtained from animals on days 11 or
16 of the luteal phase after the animals received seven days of
exogenous human CG (hCG) treatment. Examination of PKA activity in
luteal slices from various aged CL maintained in short-term organ
culture in the presence or absence of recombinant cynomolgus monkey LH
was also performed. There were no significant differences in basal or
cAMP-stimulated PKA activities in corpora lutea collected throughout
the spontaneous luteal phase. Further, Western immunoblot analyses of
the catalytic subunit of PKA (PKA C
) in corpora lutea collected
throughout the luteal phase revealed immunoreactive protein bands with
similar intensities. In vitro addition of recombinant
cynomolgus LH and dibutyryl cAMP stimulated PKA activity in corpora
lutea collected during the early, mid, and late luteal phases. In
corpora lutea obtained from animals treated with hCG during the
midluteal phase, basal PKA activity was decreased 65% as compared with
untreated day 11 controls and in late luteal phase, hCG-exposed CL
basal PKA activity was decreased 30% as compared with untreated day 16
controls. However, there were no measurable differences in
cAMP-stimulated PKA activity in CL exposed to prior hCG treatment
in vivo and Western immunoblot analyses for PKA C
in
these tissues revealed immunoreactive protein bands that were
comparable with corpora lutea collected from untreated animals.
Further, immunoblot analyses for CREB in corpora lutea collected from
hCG-treated animals revealed that CREB immunoreactivity remained
undetectable following a treatment regimen with hCG that mimics early
pregnancy. These results demonstrate that, although CREB expression
ceases following ovulation, PKA activity is maintained throughout the
luteal phase, which provides a mechanism by which the acute
steroidogenic actions of LH may be separated from longer term trophic
actions that may rely the transcriptional activity of CREB.
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