AJP - Endocrinology and Metabolism, Vol 250, Issue 1 62-E68, Copyright © 1986 by American Physiological Society
cAMP augmentation of secretagogue-induced luteinizing hormone secretion
J. L. Turgeon and D. W. Waring
Whether adenosine 3',5'-cyclic monophosphate (cAMP) acts as a mediator for
luteinizing hormone-releasing hormone (LHRH) in either its immediate LH
release action or in its self-priming action was investigated. Pituitary
pieces from either proestrous or estrous rats were superfused in vitro in
the presence of dibutyryl cAMP [(Bu)2cAMP], 8-bromo-cAMP (8BrcAMP),
forskolin, or control for 2-3 h. For proestrous but not estrous pituitary
pieces, a slight increase in base-line LH secretion rate occurred at
approximately 70 min of exposure to elevated cAMP; in the same system LHRH
caused an increase in LH secretory rate within 2 min in either proestrous
or estrous tissue. In contrast to its ineffectiveness as a secretagogue,
cAMP elevation resulted in a severalfold augmentation of both LHRH- and
elevated K+-induced LH secretion from proestrous but not estrous pituitary
pieces; for these experiments, superfusion with a cAMP analogue or
forskolin for varying times preceded a 10-min pulse of either 8 nM LHRH or
47 mM K+. Augmentation was evident after 30 min of cAMP elevation; longer
exposures were coincident with greater potentiation. Cycloheximide
prevented (Bu)2cAMP augmentation of LHRH-induced secretion. These data show
that cAMP does not mediate the immediate LH release action of LHRH, but
cAMP does augment LHRH- or K+-induced LH secretion with characteristics in
common with the self-priming action of LHRH.
