Activity-dependent feedback modulation of spike patterning of supraoptic nucleus neurons by endogenous adenosine

doi:10.1152/ajpregu.00744.2005

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Am J Physiol Regul Integr Comp Physiol 291: R83-R90, 2006. First published February 23, 2006; doi:10.1152/ajpregu.00744.2005
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Neurohypophyseal Hormones:From Genomics and Physiology to Disease

Activity-dependent feedback modulation of spike patterning of supraoptic nucleus neurons by endogenous adenosine

P. M. Bull,¹ C. H. Brown,² J. A. Russell,¹ and M. Ludwig¹

¹Centre for Integrative Physiology, University of Edinburgh, Edinburgh, United Kingdom; and ²Centre for Neuroendocrinology and Department of Physiology, Otago School of Medical Sciences, University of Otago, Dunedin, New Zealand

Submitted 20 October 2005 ; accepted in final form 17 February 2006

Neuropeptide secretion from the dendrites of hypothalamic magnocellularsupraoptic nucleus (SON) neurons contributes to the regulationof neuronal activity patterning, which ultimately determinestheir peptide output from axon terminals in the posterior pituitarygland. SON dendrites also secrete a number of other neuromodulators,including ATP. ATP degrades to adenosine in the extracellularspace to complement transported adenosine acting on pre- andpostsynaptic SON A1 receptors to reduce neuronal excitability,measured in vitro. To assess adenosine control of electricalactivity in vivo, we made extracellular single-unit recordingsof the electrical activity of SON neurons in anesthetized malerats. Microdialysis application (retrodialysis) of the A1 receptorantagonist, 8-cyclopentyl-1,3-dimethylxanthine (CPT) increasedphasic vasopressin cell intraburst firing rates progressivelyover the first 5 s by 4.5 ± 1.6 Hz (P < 0.05), andincreased burst duration by 293 ± 64% (P < 0.05).Hazard function plots were generated from interval interspikehistograms and revealed that these effects were associated withincreased postspike excitability. In contrast, CPT had no effecton the firing rates and hazard function plot profiles of continuouslyactive vasopressin and oxytocin cells. However, CPT significantlyincreased clustering of spikes, as quantified by the index ofdispersion, in oxytocin cells and continuously active vasopressincells (by 267 ± 113% and 462 ± 67%, respectively,P < 0.05). Indeed, in 4 of 5 continuously active vasopressincells, CPT induced a pseudophasic activity pattern. Together,these results indicate that endogenous adenosine is involvedin the local control of SON cell activity in vivo.

retrograde signaling; autoregulation; hypothalamus; vasopressin; oxytocin

Address for reprint requests and other correspondence: M. Ludwig, Centre for Integrative Physiology, Univ. of Edinburgh, George Square, Edinburgh EH8 9XD, UK (e-mail: mike.ludwig{at}ed.ac.uk)