Voltage‐dependent calcium channels are involved in neurogenic dural vasodilatation via a presynaptic transmitter release mechanism
- 1 October 2003
- journal article
- research article
- Published by Wiley in British Journal of Pharmacology
- Vol. 140 (3) , 558-566
- https://doi.org/10.1038/sj.bjp.0705456
Abstract
Amissense mutation of the CACNA1A gene that encodes the alpha1A subunit of the voltage-dependent P/Q-type calcium channel has been discovered in patients suffering from familial hemiplegic migraine. This suggested that calcium channelopathies may be involved in migraine more broadly, and established the importance of genetic mechanisms in migraine. Channelopathies share many clinical characteristics with migraine, and thus exploring calcium channel functions in the trigeminovascular system may give insights into migraine pathophysiology. It is also known that drugs blocking the P/Q- and N-type calcium channels have been successful in other animal models of trigeminovascular activation and head pain. In the present study, we used intravital microscopy to examine the effects of specific calcium channel blockers on neurogenic dural vasodilatation and calcitonin gene-related peptide (CGRP)-induced dilation. The L-type voltage-dependent calcium channel blocker calciseptine significantly attenuated (20 microg kg(-1), n=7) the dilation brought about by electrical stimulation, but did not effect CGRP-induced dural dilation. The P/Q-type voltage-dependent calcium channel blocker omega-agatoxin-IVA (20 microg kg-1, n=7) significantly attenuated the dilation brought about by electrical stimulation, but did not effect CGRP-induced dural dilation. The N-type voltage-dependent calcium channel blocker omega-conotoxin-GVIA (20 microg kg(-1), n=8 and 40 microg kg(-1), n=7) significantly attenuated the dilation brought about by electrical stimulation, but did not effect CGRP-induced dural dilation. It is thought that the P/Q-, N- and L-type calcium channels all exist presynaptically on trigeminovascular neurons, and blockade of these channels prevents CGRP release, and, therefore, dural blood vessel dilation. These data suggest that the P/Q-, N- and L-type calcium channels may be involved in trigeminovascular nociception.Keywords
This publication has 60 references indexed in Scilit:
- Nitric oxide synthase inhibitors can antagonize neurogenic and calcitonin gene‐related peptide induced dilation of dural meningeal vesselsBritish Journal of Pharmacology, 2002
- Functional Embryonic Cardiomyocytes after Disruption of the L-type α1C (Ca 1.2) Calcium Channel Gene in the MouseJournal of Biological Chemistry, 2000
- Dural vasodilation causes a sensitization of rat caudal trigeminal neurones in vivo that is blocked by a 5‐HT1B/1D agonistBritish Journal of Pharmacology, 1999
- The Voltage-Dependent Non-selective Cation Channel Sensitive to the L-Type Calcium Channel Blocker Efonidipine Regulates Ca2+Influx in Brain Vascular Smooth Muscle CellsBiochemical and Biophysical Research Communications, 1997
- Dopamine facilitates striatal EPSPs through an L-type Ca2+ conductanceNeuroReport, 1997
- CALCIUM CHANNEL DIVERSITY AND NEUROTRANSMITTER RELEASE: The ω-Conotoxins and ω-AgatoxinsAnnual Review of Biochemistry, 1994
- Roles of N-Type and Q-Type Ca 2+ Channels in Supporting Hippocampal Synaptic TransmissionScience, 1994
- ω-conotoxin MVIIC reversibly inhibits a human N-type calcium channel and calcium influx into chick synaptosomesNeuropharmacology, 1994
- The contribution of calcitonin gene-related peptide (CGRP) to neurogenic vasodilator responsesInflammation Research, 1993
- Vasoactive peptide release in the extracerebral circulation of humans during migraine headacheAnnals of Neurology, 1990