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Laboratory of Neuroendocrinology, Department of Biomedical Sciences, University Medical School (A.J.D., S.S., J.A.R., G.L.), Edinburgh, United Kingdom EH8 9XD; and Department of Neurobiology, The Babraham Institute (D.B.), Cambridge, United Kingdom CB2 4AT
Address all correspondence and requests for reprints to: Dr. A. J. Douglas, Laboratory of Neuroendocrinology, Department of Biomedical Sciences, University Medical School, Edinburgh, United Kingdom EH8 9XD. E-mail: alison.j.douglas{at}ed.ac.uk
Oxytocin secretion is important for the normal progress of parturition
in the rat. We tested the hypotheses that contractions of the uterus
before pup delivery activate oxytocin neurons, and that they do so via
a noradrenergic projection. In anesthetized 22-day (term) pregnant
rats, iv oxytocin pulses enhanced both uterine contractile activity and
the firing rate of oxytocin and vasopressin neurons in the supraoptic
nucleus, and these were significantly correlated. The same oxytocin
treatment also increased the expression of Fos in both the supraoptic
nucleus and the nucleus of the tractus solitarius, but not in 21-day
pregnant or virgin rats. In five of eight rats on the day of expected
parturition, noradrenaline release in the supraoptic nucleus (sampled
by microdialysis) exhibited sudden peaks during oxytocin
administration, seen in only one of nine rats given vehicle pulses.
Noradrenaline release was significantly greater in rats that went into
labor or gave birth to a pup than in rats not in labor. In rats infused
with the
1-noradrenergic receptor antagonist,
benoxathian, into the supraoptic nucleus before and during iv oxytocin
administration, Fos expression in supraoptic neurons was significantly
less than that in vehicle controls. Thus, at term pregnancy, uterine
contractions activate both oxytocin and vasopressin neurons in the SON,
and this activation involves a noradrenergic pathway.
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