Increase in plasma calcitonin gene-related peptide from the extracerebral circulation during nitroglycerin-induced cluster headache attack

Fanciullacci, M; Alessandri, Massimo; Figini, Michela; Geppetti, Pierangelo; Michelacci, S

doi:10.1016/0304-3959(94)00097-x

Cited by 249 publications

(186 citation statements)

References 31 publications

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“…This is in concert with the facial symptoms of this disorder. The findings agree well with the results of others [52] demonstrating release of CGRP in nitroglycerin-elicited attacks of cluster headache. Fanciullacci et al [53] observed in another study that nitroglycerin could only elicit an attack of cluster headache with CGRP release if the patient was in a latent period and thus prone to activation.…”

Section: Cluster Headachesupporting

confidence: 93%

Sensory nerves in the human cerebral circulation and trigeminal ganglion: role in primary headaches

Edvinsson

2002

J Headache Pain

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IntroductionWith the advances in the understanding of cranial pain processing that have been made over the last few years it has become clear that cranial vessels have an important role in the expression of vascular pain syndromes such as migraine and cluster headache. Recent data show that specific populations of cerebrovascular sensory nerves are involved in the pathophysiology of these pain syndromes. The present review provides an account of my interpretation of available data on perivascular peptides in the pathogenesis of primary headaches. This includes a detailed description of the human cerebrovascular sensory innervation, the origin, immunocytochemical distribution and ultrastructural features of perivascular nerves and their role in primary headaches. A general view of the pathophysiologyCurrent data provide a model in which a central "generator", different in migraine ( Fig. 1) and in cluster headache, is activated. This may initiate a wave of "spreading depression" or vasoconstriction via amine-containing fibers originating in the brain stem [1]. Following alteration of cerebral blood vessel tone, the trigeminovascular reflex [2] is initiated to counter-balance cerebrovascular constriction, in part via release of calcitonin gene-related peptide (CGRP) and vasoactive intestinal peptide (VIP). The study of neuropeptide levels in migraine and cluster headache is now providing a link between clinical and basic research that is so crucial if the pathophysiology is to be understood (for more details see [3]). In migraine (with and without aura), marked Lars EdvinssonAbstract Our knowledge of the nervous control of the cerebral circulation has increased by the use of denervations and retrograde tracing in combination with immunohistochemical techniques. We have demonstrated that cerebral vessels are supplied with sensory nerve fibers containing a multiplicity of transmitter substances originating in the trigeminal ganglion. The majority of these transmitters are neuropeptides, but the gaseous signal substance, nitric oxide (NO), is also included. In primary headaches, calcitonin generelated peptide (CGRP) is released in parallel with the headache, while the parasympathetic nerve transmitter vasoactive intestinal peptide (VIP) is released in parallel with facial symtoms. Thus, the perivascular nerves participate in the pathogenesis of primary headaches. Current migraine drugs, e.g. triptans, act in part by inhibiting the release of CGRP from the sensory nerves.

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Section: Cluster Headachesupporting

confidence: 93%

Sensory nerves in the human cerebral circulation and trigeminal ganglion: role in primary headaches

Edvinsson

2002

J Headache Pain

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“…*p Ͻ 0.05. ric [Ca 2ϩ ] i measurements revealed involvement of SNAP-25 in spontaneous and evoked CGRP exocytosis, with important implications for synaptic communication between trigeminal sensory neurons. In light of the well established proinflammatory activity of CGRP and its direct involvement in migraine (Fanciullacci et al, 1995;Doods et al, 2007), our data yield new information pertinent to the mechanism of chronic pain and provide a scientific basis for using BoNT variants as therapeutics for chronic pain and neuroinflammatory disorders.…”

Section: Discussionmentioning

confidence: 81%

Activation of TRPV1 Mediates Calcitonin Gene-Related Peptide Release, Which Excites Trigeminal Sensory Neurons and Is Attenuated by a Retargeted Botulinum Toxin with Anti-Nociceptive Potential

Meng¹,

Ovsepian²,

Wang³

et al. 2009

J. Neurosci.

220

193

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“…Thus, BIBN4096BS could produce, at a postjunctional level (by CGRP receptor blockade), effects similar to those that triptans cause by reducing CGRP release, and that result in inhibition of CGRP receptor signalling. Indeed, triptans inhibit trigeminal CGRP release in animal experimental models [55,63], and clinical data show that sumatriptan normalised the elevated CGRP levels with alleviation of migraine [55] and cluster headache attack [65]. These findings have suggested that BIBN4096BS could be developed as an effective antimigraine drug.…”

Section: Cgrp Antagonists In Migrainementioning

confidence: 97%

“…A Ca 2+ -dependent and capsaicin-sensitive release of CGRP, but not SP, has been documented from human tissues containing non-trigeminal [13] or trigeminal [11] sensory nerve endings. Furthermore, plasma concentrations of CGRP, but not of SP, were elevated during the headache phase of migraine [64] and cluster headache [65]. There is evidence that intravenous infusion of CGRP produces a migraine-like headache [66], and intravenous infusion of nitric oxide produces a migraine-like headache with an associated increase in plasma CGRP levels [67].…”

Section: Migraine and Neurogenic Inflammationmentioning

confidence: 99%

CGRP and migraine: neurogenic inflammation revisited

Geppetti

Capone²,

Trevisani

et al. 2005

J Headache Pain

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The term 'neurogenic inflammation' refers to a series of proinflammatory responses produced by the stimulation of peripheral terminals of a subset of primary sensory neurons and the subsequent release of the neuropeptides, calcitonin gene-related peptide (CGRP) and the tachykinins, substance P (SP) and neurokinin A (NKA) [1]. The neurons that produce inflammation comprise a heterogeneous cell population with A-delta and C fibres, defined as polymodal nociceptors because they sense thermal, chemical and high-threshold mechanical stimuli. These neurons express on their plasma membrane a large panel of excitatory and inhibitory receptors and channels, and some of these signalling proteins have been successfully used as targets for analgesic or anti-inflammatory drugs. Among the channels expressed on peptidergic primary sensory neurons, transient receptor potential vanilloid-1 (TRPV1) [2], activated by the xenobiotic capsaicin, the pungent ingredient of plants of the genus Capsicum, is of paramount importance. Capsaicin produces burning pain by stimulating TRPV1 and by releasing sensory neuropeptides causes neurogenic inflammation. However, high concentrations/doses of capsaicin have the ability, after an initial excitatory phase, to desensitise the sensory nerve terminals, thus reducing the transmission of sensory/pain signals and abolishing neurogenic inflammation [3, 4]. This specific feature of capsaicin has greatly contributed to define the role of this subset of sensory nerves in pathophysiological models of human diseases and has been Pierangelo Geppetti Jay Guido Capone Marcello Trevisani Paola Nicoletti Giovanni Zagli Maria Rosalia Tola Abstract For more than a century neurogenic inflammation has been proposed to have a role in various human diseases. The present review will cover the conceptual steps of the itinerary that has led to the conclusion that neurogenic inflammation is important in migraine. Of particular relevance for the object of this article is the observation that tachykinindependent neurogenic inflammatory responses are evident in rodents, but much less pronounced or absent in other mammal species, including man, whereas neurogenic vasodilatation, most likely mediated by CGRP, occurs in most mammalian species and also in man. Recent evidence that a CGRP receptor antagonist was effective in the treatment of migraine attack supports the hypothesis that neurogenic vasodilatation is a major underlying mechanism of migraine.

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Increase in plasma calcitonin gene-related peptide from the extracerebral circulation during nitroglycerin-induced cluster headache attack

Cited by 249 publications

References 31 publications

Sensory nerves in the human cerebral circulation and trigeminal ganglion: role in primary headaches

Sensory nerves in the human cerebral circulation and trigeminal ganglion: role in primary headaches

Activation of TRPV1 Mediates Calcitonin Gene-Related Peptide Release, Which Excites Trigeminal Sensory Neurons and Is Attenuated by a Retargeted Botulinum Toxin with Anti-Nociceptive Potential

CGRP and migraine: neurogenic inflammation revisited

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