Post-stimulus potentiation of transmission in pelvic ganglia enhances sympathetic dilatation of guinea-pig uterine artery in vitro

Vasodilatation produced by stimulation of preganglionic neurones in lumbar and sacral pathways to pelvic ganglia was studied using an in vitro preparation of guinea-pig uterine artery and associated nerves in a partitioned bath allowing selective drug application to the ganglia or artery. Arterial d...

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Bibliographic Details
Published in:The Journal of physiology 2005-07, Vol.566 (1), p.189-203
Main Authors: Morris, Judy L., Gibbins, Ian L., Jobling, Phillip
Format: Article
Language:English
Subjects:
Animals
Arteries - innervation
Arteries - physiology
Electric Stimulation - methods
Female
Ganglia, Autonomic - physiology
Ganglia, Spinal - physiology
Guinea Pigs
In Vitro Techniques
Long-Term Potentiation - physiology
Neuronal Plasticity - physiology
Pelvis - innervation
Pelvis - physiology
Synaptic Transmission - physiology
Tissue, System and Organ Physiology
Uterus - blood supply
Uterus - innervation
Uterus - physiology
Vasodilation - physiology
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Summary:Vasodilatation produced by stimulation of preganglionic neurones in lumbar and sacral pathways to pelvic ganglia was studied using an in vitro preparation of guinea-pig uterine artery and associated nerves in a partitioned bath allowing selective drug application to the ganglia or artery. Arterial diameter was monitored using real time video imaging. Vasodilatations produced by hypogastric nerve stimulation (HN; 300 pulses, 10 Hz) were significantly larger and longer in duration than with pelvic nerve stimulation ( N = 18). Stimulation of ipsilateral lumbar splanchnic nerves or ipsilateral third lumbar ventral roots also produced prolonged vasodilatations. Blockade of ganglionic nicotinic receptors (0.1–1 m m hexamethonium) delayed the onset and sometimes reduced the peak amplitude of dilatations, but slow dilatations persisted in 16 of 18 preparations. These dilatations were not reduced further by 3 μ m capsaicin applied to the artery and ganglia, or ganglionic application of 1 μ m hyoscine, 30–100 μ m suramin or 10 μ m CNQX. Dilatations were reduced slightly by ganglionic application of NK1 and NK3 receptor antagonists (SR140333, SR142801; 1 μ m ), but were reduced significantly by bathing the ganglia in 0.5 m m Ca 2+ and 10 m m Mg 2+ . Intracellular recordings of paracervical ganglion neurones revealed fast excitatory postsynaptic potentials (EPSPs) in all neurones on HN stimulation (300 pulses, 10 Hz), and slow EPSPs (3–12 mV amplitude) in 25 of 37 neurones. Post-stimulus action potential discharge associated with slow EPSPs occurred in 16 of 37 neurones (firing rate 9.4 ± 1.5 Hz). Hexamethonium (0.1–1 m m ) abolished fast EPSPs. Hexamethonium and hyoscine (1 μ m ) did not reduce slow EPSPs and associated post-stimulus firing in identified vasodilator neurones (with VIP immunoreactivity) or non-vasodilator paracervical neurones. These results demonstrate a predominantly sympathetic origin of autonomic pathways producing pelvic vasodilatation in females. Non-cholinergic mediators of slow transmission in pelvic ganglia produce prolonged firing of postganglionic neurones and long-lasting dilatations of the uterine artery. This mechanism would facilitate maintenance of pelvic vasodilatation on stimulation of preganglionic neurones during sexual activity.
ISSN:0022-3751
1469-7793
DOI:10.1113/jphysiol.2005.083493