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Chan SL, Fiscus RR. Mol Hum Reprod. 2003 Dec;9(12):775-83
Guanylyl cyclase inhibitors NS2028 and ODQ and protein
kinase G (PKG) inhibitor KT5823 trigger apoptotic DNA
fragmentation in immortalized uterine epithelial cells:
anti-apoptotic effects of basal cGMP/PKG
Department of Physiology (Faculty of Medicine), Epithelial
Cell Biology Research Centre and Centre for Gerontology and
Geriatrics, The Chinese University of Hong Kong, Shatin, New
Territories, Hong Kong, China.
The cGMP/protein kinase G (PKG) signalling pathway, at basal
levels, has anti-apoptotic/pro-survival effects in certain
neural cells. The present study determined apoptosis-regulating
effects of basal cGMP/PKG in an immortalized uterine epithelial
cell line, HRE-H9 cells, using two soluble guanylyl cyclase (sGC)
inhibitors, NS2028 and ODQ, and a PKG inhibitor, KT5823. A new
quantitative, ultrasensitive technique using capillary
electrophoresis with laser-induced fluorescent detector (CE-LIF),
recently developed in our laboratory, was used to quantify
levels of apoptotic DNA fragmentation. NS2028 and ODQ increased
apoptotic DNA fragmentation by 3.5- and 9-fold respectively,
suggesting that lowering basal cGMP levels causes spontaneous
apoptosis. 8-Br-cGMP, a cell-permeable cGMP analogue that
directly activates PKG, reduced ODQ-induced apoptosis by 81%,
indicating that replacement of lowered cGMP with a direct PKG
activator prevents apoptosis. Western blot analysis, using PKG
type I (PKG-I)-specific antibody, indicated that HRE-H9 cells
express PKG-I at moderate levels. Inhibiting basal PKG activity
with KT5823 increased apoptotic DNA fragmentation by 9.8-fold.
Overall, the data show that inhibitors of basal sGC and PKG
activities in immortalized uterine epithelial cells cause
apoptosis, suggesting that normal basal levels of cGMP and PKG
activity may be necessary to prevent a spontaneous development
of apoptosis in these cells.
PMID: 14614039 |
