2007
DOI: 10.1016/j.pain.2006.09.039
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Immunohistochemical localization of histamine H3 receptors in rodent skin, dorsal root ganglia, superior cervical ganglia, and spinal cord: Potential antinociceptive targets

Abstract: Activation of histamine H 3 receptors (H 3 Rs) reduces inflammation and nociception, but the existence of H 3 Rs on peripheral innervation has never been demonstrated. Here we use antibodies to locate H 3 Rs in whisker pads, hairy and glabrous hind paw skin, dorsal root ganglia (DRGs), and spinal cords of rats, wild-type mice, and H 3 R knockout (H 3 KO) mice. Although H 3 Rs have been hypothesized to be on C and sympathetic fibers, H 3 R-like immunoreactivity (H 3 R-LI) was only detected on presumptive periar… Show more

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Cited by 82 publications
(89 citation statements)
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“…injection of histamine induces CGRP release into the CSF (Bileviciute et al, 1994) and (iii) histamine administered to the nasal mucosa causes CGRP release from the peripheral terminals of trigeminal ganglion in the guinea pig (Tani et al, 1990). Further support for this link between histamine and CGRP is attained from the observed co-localization of the histamine H3 receptor with CGRP on Aδ fibres, with both mediators contributing to a high-threshold mechanical nociceptive effect (Cannon et al, 2007).…”
Section: Histamine Neurogenic Inflammation and Nociceptive Painmentioning
confidence: 97%
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“…injection of histamine induces CGRP release into the CSF (Bileviciute et al, 1994) and (iii) histamine administered to the nasal mucosa causes CGRP release from the peripheral terminals of trigeminal ganglion in the guinea pig (Tani et al, 1990). Further support for this link between histamine and CGRP is attained from the observed co-localization of the histamine H3 receptor with CGRP on Aδ fibres, with both mediators contributing to a high-threshold mechanical nociceptive effect (Cannon et al, 2007).…”
Section: Histamine Neurogenic Inflammation and Nociceptive Painmentioning
confidence: 97%
“…It is possible that these histamine H3 receptor antagonists block the modulatory role of the presynaptic H3 receptor, thus favouring the release of neuropeptides from sensory endings (Cannon et al, 2007). More recently, data obtained with clobenproprit, an H3 receptor antagonist and H4 receptor agonist, suggest that the H4 receptor is also involved in itch.…”
Section: Histamine and Neurogenic Inflammation In The Skinmentioning
confidence: 99%
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“…164) In contrast to the latter, GSK334429 is a less rigidized 1,4-diazepane possessing comparable properties to that of GSK189254. It is active in attention and cognition models but what is more important, both, GSK189254 and GSK334429, have recently shown to be efficacious in models of neuropathic pain 165) pointing out a possible additive indication for these short-acting and poor brain penetrating ligands as H 3 R modulates pain reception in the dorsal horn and spinal cord 48) (Fig. 7, Tables 1, 2).…”
Section: )mentioning
confidence: 99%
“…28) H 3 R expression is not solely restricted to histaminergic neurons: due to its function as a heteroreceptor it can be found on colocalised neurons, and H 3 R activation modulates the release of various important neurotransmitters, i.e. dopamine, [29][30][31][32][33] acetylcholine, [34][35][36][37] norepinephrine, 38,39) serotonin, 40,41) GABA, [42][43][44] glutamate, 45) and substance P. [46][47][48] Therefore, histaminergic neurons and the cross-linkage between major neurotransmitter systems are involved in many (patho)physiological brain functions, including vigilance, memory processes, feeding behaviour and locomotor activity (Fig. 2).…”
mentioning
confidence: 99%