Release of Oxytocin into Blood and into Cerebrospinal Fluid Induced by Naloxone in Anaesthetized Morphine-Dependent Rats: The Role of the Paraventricular Nucleus

Opioid actions on oxytocin secretion into blood and cerebrospinal fluid (CSF) were investigated in urethane‐anaesthetized female rats after intracerebroventricular (icv) infusion of morphine sulphate or vehicle for 5 days. Serial femoral arterial blood samples and cisterna magna CSF samples were col...

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Published in:Journal of neuroendocrinology 1991-10, Vol.3 (5), p.551-561
Main Authors: Coombes, J. E., Robinson, I. C. A. F., Antoni, F. A., Russell, J. A.
Format: Article
Language:English
Subjects:
Biological and medical sciences
cerebrospinal fluid
Fundamental and applied biological sciences. Psychology
Hormones and neuropeptides. Regulation
Hypothalamus. Hypophysis. Epiphysis. Urophysis
morphine-dependence
oxytocin
paraventricular nucleus
pituitary stress hormones
Vertebrates: endocrinology
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Summary:Opioid actions on oxytocin secretion into blood and cerebrospinal fluid (CSF) were investigated in urethane‐anaesthetized female rats after intracerebroventricular (icv) infusion of morphine sulphate or vehicle for 5 days. Serial femoral arterial blood samples and cisterna magna CSF samples were collected for radioimmunoassay. Naloxone was given to assess endogenous opioid tone in icv vehicle‐infused rats and to precipitate withdrawal in morphine‐dependent animals. Initial plasma oxytocin concentration was not affected by icv morphine infusion. In control rats receiving icv vehicle, naloxone increased plasma oxytocin 11‐fold within 5 min, and in icv morphine‐infused rats, naloxone increased plasma oxytocin 80‐fold within 5 min. In both groups, 90 min after naloxone plasma oxytocin was still 5 and 10 times, respectively, the initial concentration. Without naloxone, neither plasma nor CSF oxytocin concentration changed significantly with time (up to 90 min) in either icv treatment group. In the icv vehicle group, there was a 2‐fold increase in CSF oxytocin 90 min after naloxone. In the icv morphine‐infused group, CSF oxytocin was increased 5‐fold 40 min after naloxone. In another group of icv morphine‐infused rats, intravenous infusion of oxytocin to achieve plasma levels similar to those seen after naloxone, did not significantly increase CSF oxytocin. In a further group of icv morphine‐infused rats, [3H]oxytocin was infused intravenously immediately after naloxone was given; in these rats oxytocin transfer from blood to CSF could account at most for only 20% of the increase in CSF oxytocin after naloxone. A further group of rats underwent bilateral microknife ablation of the paraventricular nuclei (PVN) 9 days before icv vehicle or morphine infusions were started; blood and CSF samples were collected under urethane anaesthesia. Initial concentrations of oxytocin in CSF and in plasma were similar in both groups with PVN ablation. In all PVN‐lesioned rats initial plasma concentrations of oxytocin were undetectable (
ISSN:0953-8194
1365-2826
DOI:10.1111/j.1365-2826.1991.tb00316.x