The 5-HT2A receptor has been shown to be widely distributed throughout the spinal cord and is present at presynaptic and postsynaptic sites therein. This receptor subtype shows dense labelling in lamina II inner and is therefore ideally located for modulation of spinal nociceptive processing. With regards to primary afferent neurones, 5-HT2A receptors are mainly localised in small and medium sized DRG neurones with most 5-HT2A receptor immunolabeled cells expressing the TRPV1 receptor, thus indicating their nociceptive selleck screening library nature (Doly et
al., 2004 and Van Steenwinckel et al., 2009). It is a G-protein coupled receptor positively coupled to phospholipase C, leading to an increase in phosphotidylinositol and intracellular calcium. In vitro electrophysiological recordings have shown a long lasting synaptic facilitation of superficial dorsal horn neurones mediated by 5-HT acting at 5-HT2 receptors ( Hori et al., 1996). Taken together, these data would
implicate an excitatory role for the 5-HT2A receptor in spinal nociceptive transmission. The findings from behavioural studies are mixed. For instance, spinal administration of the mixed 5-HT2A/C agonist, (±)-2,5-dimethoxy-4-iodoamphetamine, (DOI), increased the behavioural response to formalin injection, an effect reversed by ketanserin (Kjorsvik et al., 2001), and DOI induced pain-like behaviours such as licking and biting, in line with a pronociceptive role for 5-HT2 receptors (Eide and Hole, 1991). Similarly, blocking spinal check details 5-HT2A receptors inhibited the formalin response (Nishiyama,
2005) and reduced spinal FOS activation in a paw incision model (Silveira et al., 2010). In direct contrast to the aforementioned studies, intrathecal administration of 5-HT2A/2C receptor agonists reversed the behavioural pain-like responses to formalin and chronic constriction nerve injury. These effects were reversed by pretreatment with intrathecal administration of ketanserin, therefore implicating spinal 5-HT2A receptors in mediating the antinociceptive effects of 5-HT (Sasaki et al., 2001 and Sasaki et al., 2003), and 5-HT2A receptor induced spinal acetylcholine release and consequent antinociception was demonstrated (Kommalage oxyclozanide and Hoglund, 2005) In rat models of chemotherapy and HIV-therapy induced neuropathy, however, a significant increase in 5-HT2AR immunoreactivity was seen in the superficial layers of the lumbar dorsal horn and an epidural injection of a selective 5-HT2A receptor antagonist dose-dependently decreased the thermal and mechanical hypersensitive behaviours; furthermore 5-HT2A receptor knockout mice did not develop HIV-therapy or chemotherapy-induced neuropathic pain behaviours whereas control littermates displayed a neuropathy comparable to that observed in rats (Thibault et al., 2008).
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