Iwagaki, N., Ganley, R. P., Dickie, A., Polgár, E., Hughes, D. I. , Del Rio, P., Revina, Y., Watanabe, M., Todd, A. J. and Riddell, J. S. (2016) A combined electrophysiological and morphological study of NPY-expressing inhibitory interneurons in the spinal dorsal horn of the mouse. Pain, 157(3), pp. 598-612. (doi: 10.1097/j.pain.0000000000000407) (PMID:26882346) (PMCID:PMC4751741)
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Abstract
The spinal dorsal horn contains numerous inhibitory interneurons that control transmission of somatosensory information. Although these cells have important roles in modulating pain, we still have limited information about how they are incorporated into neuronal circuits, and this is partly due to difficulty in assigning them to functional populations. Around 15% of inhibitory interneurons in laminae I-III express neuropeptide Y (NPY), but little is known about this population. We therefore used a combined electophysiological/morphological approach to investigate these cells in mice that express green fluorescent protein (GFP) under control of the NPY promoter. We show that GFP is largely restricted to NPY-immunoreactive cells, although it is only expressed by a third of those in lamina I-II. Reconstructions of recorded neurons revealed that they were morphologically heterogeneous, but never islet cells. Many NPY-GFP cells (including cells in lamina III) appeared to be innervated by TRPV1-lacking C fibres, and consistent with this, we found that some lamina III NPY-immunoreactive cells were activated by mechanical noxious stimuli. Projection neurons in lamina III are densely innervated by NPY-containing axons. Our results suggest that this input originates from a small subset of NPY-expressing interneurons, with the projection cells representing only a minority of their output. Taken together with results of previous studies, our findings indicate that somatodendritic morphology is of limited value in classifying functional populations among inhibitory interneurons in the dorsal horn. Since many NPY-expressing cells respond to noxious stimuli, these are likely to have a role in attenuating pain and limiting its spread.
Item Type: | Articles |
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Status: | Published |
Refereed: | Yes |
Glasgow Author(s) Enlighten ID: | Hughes, Dr David I and Iwagaki, Mr Noboru and Beresford-Polgar, Dr Erika and Todd, Professor Andrew and Del Rio, Dr Patricia and Dickie, Dr Allen and Riddell, Professor John |
Authors: | Iwagaki, N., Ganley, R. P., Dickie, A., Polgár, E., Hughes, D. I., Del Rio, P., Revina, Y., Watanabe, M., Todd, A. J., and Riddell, J. S. |
College/School: | College of Medical Veterinary and Life Sciences > School of Psychology & Neuroscience |
Journal Name: | Pain |
Publisher: | Lippincott Williams & Wilkins |
ISSN: | 0304-3959 |
ISSN (Online): | 1872-6623 |
Copyright Holders: | Copyright © 2015 The Authors |
First Published: | First published in Pain 157(3):598-612 |
Publisher Policy: | Reproduced under a Creative Commons License |
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