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Biology of Reproduction, Vol 23, 963-973, Copyright © 1980 by Society for the Study of Reproduction
1 Department of Physiology,
University of Texas Health Science Center,
Dallas, Texas 75235 The sequential inhibitory effect of progesterone (P) may represent a model of how P acts to
terminate sexual receptivity in the rodent. In the present studies, the sequential inhibitory effect of
P on lordotic responsiveness was demonstrated in ovariectomized rats bearing Silastic capsules of
estradiol (E2) for 48 h and injected with P 3 h after E2 removal and again 24 h later. In a time
course study, inhibition of hordotic responsiveness was evident 18 h following continuous exposure
to P, establishing that P requires a relatively long time-interval to develop its inhibitory effect on
lordotic responsiveness. The RNA synthesis inhibitor actinomycin-D infused intraventricularly into
E2-primed rats at the time of the first of two P injections did not prevent the appearance of the
sequential inhibitory effect of P, suggesting that despite the long time-interval required for the
development of P inhibition of sexual behavior, new RNA synthesis is not required. Results of the
present studies also show that the continued presence of E2 for 11 h or more following the first of
two P injections prevents the appearance of (nullifies) the sequential inhibitory effect of P, confirming and extending previous reports that estrogen can interfere with the development of the
sequential inhibitory effect of P.
Note:
ACKNOWLEDGMENTS
The technical assistance of Mr. George Crowley
and Mrs. Loretta Dice in performing steroid assays is
appreciated.
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