Author:
Brooks A. N.,Challis J. R. G.
Abstract
ABSTRACT
To test the hypothesis that endogenous opioids participate in the regulation of the ontogenic development of the hypothalamic-pituitary-adrenal axis in fetal sheep, we measured changes in immunoreactive (ir) ACTH and cortisol concentrations in response to bolus injections of either the [Met]-enkephalin analogue, [d-Ala2,N-Phe4,Met(0)ol5]-enkephalin (FK 33-824; 25 μg), the opioid antagonist naloxone (1 mg), a combination of both, or saline vehicle, administered to chronically catheterized fetal sheep through late gestation.
There were no effects of either FK 33-824, naloxone or saline on the release of ir-ACTH and cortisol at the earliest stage of gestation studied (days 110–115). By days 125–130, FK 33-824 caused a rapid but short-lived (30 min) increase in plasma ir-ACTH (P <0·05) which was accompanied by a smaller but nonsignificant increase in cortisol. Naloxone given concurrently with FK 33-824 abolished this response, thus providing evidence for a specific effect through opioid receptors. Naloxone given alone was without effect. At days 135–140, FK 33-824 caused a significant increase in ir-ACTH which was of similar duration and magnitude to that which occurred at days 125–130. There was a larger basal variation in plasma concentrations of cortisol than at days, 125–130, and a greater increase in cortisol after FK 33-824, although this did not reach statistical significance. Naloxone again reversed the effects of FK 33-824 but was without effect when given alone.
We conclude that opioid receptors capable of mediating the effects of exogenously administered opioid peptides on the pituitary-adrenal axis are present in fetal sheep by days 123–130. However, we have been unable to demonstrate tonic control of this axis by endogenous opioids, since naloxone is ineffective when given alone.
J. Endocr. (1988) 119, 389–395
Subject
Endocrinology,Endocrinology, Diabetes and Metabolism
Cited by
18 articles.
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