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Depression of sympathetic preganglionic neurons by clonidine: evidence for stimulation of 5-HT receptors

Authors :
Robert J. Neumayr
Donald N. Franz
Bradford D. Hare
Source :
Clinical and experimental hypertension. 1(1)
Publication Year :
1978

Abstract

In unanesthetized spinal cats, clonidine HCl (5-50 microgram/kg, i.v.) rapidly and markedly depressed excitatory transmission through two spinal pathways to sympathetic preganglionic neurons. Depression through either pathway was dose-dependent and persisted for more than 3 hr but could be rapidly antagonized at any stage by tolazoline HCl in a dose-ratio of about 1:100. The two spinal pathways were also depressed transiently by L-dopa and for prolonged periods by 5-HTP; both precursors were shown to act by releasing 5-HT from bulbospinal 5-HT terminals and their depressant effects were also antagonized by tolazoline. In the absence of 5-HT-induced depression, L-dopa only enhanced transmission through both pathways by inducing release of catecholamines from bulbospinal NE terminals. These results indicate that clonidine depresses sympathetic activity by stimulating inhibitory 5-HT receptors on sympathetic preganglionic neurons, a mechanism that adequately accounts for its central vasodepressor effect.

Details

ISSN :
01483927
Volume :
1
Issue :
1
Database :
OpenAIRE
Journal :
Clinical and experimental hypertension
Accession number :
edsair.doi.dedup.....0940f2f6ead7bcb43cad9a26eecaa1dc