Response Properties of Dural Nociceptors in Relation to Headache.
From: Dept. of Anesthesia, DA-717, Beth Israel Deaconess Med. Ctr., 330 Brookline Ave., Boston, MA 02215, USA. Andrew_Strassman@bidmc.harvard.edu
Journal of neurophysiology
- Publish Date: Mar 2006
- ISSN: 0022-3077
- Volume: 95
- Issue: 3
- Pages: 1298-306
- Medium: Print
- Language: English
- Citation (JAMA): Strassman Andrew M, Levy Dan, et al. Response Properties of Dural Nociceptors in Relation to Headache.. J. Neurophysiol. Mar 2006;95:1298-306
Abstract
Single-unit electrophysiological recording studies have examined the activity of sensory neurons in the trigeminal ganglion that innervate the intracranial meninges to better understand their possible role in headache. A key question is whether the meningeal sensory neurons are similar to nociceptive neurons in other tissues or, alternatively, whether they have unique properties that might be of significance for headache pathogenesis and drug therapy. Such studies have indeed found that the intracranial dura is innervated by neurons that exhibit properties characteristic of nociceptors in other tissues, including chemosensitivity and sensitization. This sensitization, consisting of an enhanced responsiveness to mechanical stimuli, might be relevant to symptoms that are characteristic of certain headaches that indicate the presence of an exaggerated intracranial mechanosensitivity. Studies that examined whether the anti-migraine agent sumatriptan might inhibit this sensitization (in addition to its well-known inhibition of neurotransmitter release) found that it had no inhibitory effect but rather produced a calcium-dependent discharge, which might account for the initial worsening of headache that can follow sumatriptan administration. In studies that examined the effects of vasodilator agents, nitroprusside produced mixed effects on mechanosensitivity, whereas calciton gene-related peptide (CGRP) had no effect on either spontaneous or mechanically evoked discharge. These results call into question the role of vasodilation in headache and suggest that the role of CGRP in headache may be through its action as a central neurotransmitter rather than through vasodilation and activation of meningeal nociceptors. In general, studies of meningeal sensory neurons have not found evidence of unique properties that distinguish them from nociceptive neurons in other tissues. Ultimately the distinctive clinical characteristics of headache may prove to be related not so much to any differences in the intrinsic molecular or cellular properties of the meningeal sensory neurons but rather to the distinctive properties of the tissue that they innervate.
Mesh Headings (Keywords): Animals, Dura Mater, Humans, Mechanotransduction, Cellular, Nociceptors, Pain, Pain Threshold, Trigeminal Ganglion
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