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Original Articles |
1
Department of Obstetrics and Gynecology, University of British Columbia, Vancouver, British Columbia, Canada V6H 3V5; and Taipei Medical College Hospital (C.-J.T., C.-R.T.), 110 Taipei, Taiwan
Address all correspondence and requests for reprints to: Dr. Peter C. K. Leung, Department of Obstetrics and Gynecology, University of British Columbia, Room 2H30, 4490 Oak Street, Vancouver, British Columbia, Canada V6H 3V5. E-mail: peleung{at}interchange.ubc.ca
Abstract
The presence of P2U purinoceptor in human granulosa-luteal cells
(hGLCs) indicates a potential role of ATP in regulating ovarian
function. In this study an inhibitory effect of ATP on hCG-induced cAMP
production was observed. Extracellular ATP has been shown to activate
protein kinase C (PKC) after binding to a purinoceptor. To understand
the role of PKC in mediating ATP action, hCG-stimulated cAMP level was
examined in the presence of the PKC activator, 1 µmol/L phorbol
12-myristate 13-acetate (PMA), or the PKC inhibitor, 1 µmol/L
staurosporin or 1 µmol/L bisindolylmaleimide I. PMA, like 10 µmol/L
ATP, significantly reduced hCG-evoked cAMP production. In addition, the
inhibitory effect of ATP was reversed by staurosporin and
bisindolylmaleimide I. To further investigate the involvement of PKC
isoforms in mediating the inhibitory effect of ATP, the presence of PKC
isoforms in cultured hGLCs was examined by Western blot using
monoclonal antibodies against specific isoforms. Translocation of PKC
isoforms from cytosolic fraction to membrane fraction was studied to
identify the active PKC isozymes subsequent to ATP treatment. The
change in PKC isoform in PKC-depleted cells (achieved by exposure to
PMA for 18 h) was also examined. Our results demonstrated the
presence of PKC
, -
, -
, and -
isoforms in hGLCs and the
translocation of PKC subsequent to ATP treatment. In
PKC-depleted cells the PKC level was reduced, and no significant
effect of ATP on hCG-stimulated cAMP production was observed. To our
knowledge, this is the first demonstration of PKC isoforms in hGLCs and
the involvement of activated PKC in mediating the antigonadotropic
effect of extracellular ATP. Taken together, these results further
support a role of this neurotransmitter in regulating human ovarian
function.
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