| Literature DB >> 20497578 |
Ewan St John Smith1, Gregory R C Blass, Gary R Lewin, Thomas J Park.
Abstract
Recent research has proposed a pathway in which sensory neurons expressing the capsaicin activated ion channel TRPV1 are required for histamine-induced itch and subsequent scratching behavior. We examined histamine-induced itch in the African naked mole-rat (Heterocephalus glaber) and found that although naked mole-rats display innate scratching behavior, histamine was unable to evoke increased scratching as is observed in most mouse strains. Using calcium imaging, we examined the histamine sensitivity of naked mole-rat dorsal root ganglia (DRG) neurons and identified a population of small diameter neurons activated by histamine, the majority of which are also capsaicin-sensitive. This suggested that naked mole-rat sensory neurons are activated by histamine, but that spinal dorsal horn processing of sensory information is not the same as in other rodents. We have previously shown that naked mole-rats naturally lack substance P (SP) in cutaneous C-fibers, but that the neurokinin-1 receptor is expressed in the superficial spinal cord. This led us to investigate if SP deficiency plays a role in the lack of histamine-induced scratching in this species. After intrathecal administration of SP into the spinal cord we observed robust scratching behavior in response to histamine injection. Our data therefore support a model in which TRPV1-expressing sensory neurons are important for histamine-induced itch. In addition, we demonstrate a requirement for active, SP-induced post-synaptic drive to enable histamine sensitive afferents to drive itch-related behavior in the naked mole-rat. These results illustrate that it is altered dorsal horn connectivity of nociceptors that underlies the lack of itch and pain-related behavior in the naked mole-rat.Entities:
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Year: 2010 PMID: 20497578 PMCID: PMC2886013 DOI: 10.1186/1744-8069-6-29
Source DB: PubMed Journal: Mol Pain ISSN: 1744-8069 Impact factor: 3.395
Figure 1Spontaneous and histamine-induced scratching in naked mole-rats compared to laboratory mice. , Mice and naked mole-rats use their back legs to scratch their bodies at a low spontaneous level. The bar graph shows the average number of bouts of scratching observed over 20 minutes (n = 16 mice; 16 naked mole-rats). , Histamine is not pruritogenic in naked mole-rats. For mice, 10 μg histamine failed to evoke scratching, but higher doses (20 μg - 4.6 mg) evoked pronounced scratching. In contrast, none of the doses tested induced scratching in naked mole-rats.
Figure 2Histamine activates naked mole-rat DRG neurons. , pie-chart showing different populations of DRG neurons, 10% (n = 35/343) were activated by 1 μM capsaicin, 10% by 100 μM histamine (n = 35/343), 13% were activated by both stimuli (n = 45/343). , example traces showing the time-course of experiments and the different response types. , groups of neurons responding to either capsaicin, histamine or both were significantly smaller than the group which was not activated by either stimulus (**, p < 0.01 and ***, p < 0.001). Results are taken from 5 different DRG neuron cultures.
Figure 3Substance P "rescues" histamine-mediated scratching in naked mole-rats. , naked mole-rats: after intrathecal administration of saline, intracutaneous histamine fails to evoke any more scratching than saline (black bar vs. grey bar), however after intrathecal SP treatment, histamine evokes robust scratching (red bar). Intrathecal administration of SP alone (green bar) increases scratching compared to spontaneous levels (blue bar), but combining intrathecal SP with subsequent intracutaneous saline induces no greater effect (yellow bar). , mice: intracutaneous histamine causes increased scratching (black bar) compared to saline alone (grey bar) and is of a similar magnitude following intrathecal SP treatment (red bar). Intrathecal SP administration induces more scratching than is observed spontaneously (green vs. blue bar), but combining intrathecal SP with subsequent intracutaneous saline induces no greater effect (yellow bar). N = 4 animals for each group; it/ic, intrathecal treatment/intracutaneous treatment; sal, saline, hist, histamine, SP, substance P, spont, spontaneous and *, p < 0.05, **, p < 0.01 and ***, p < 0.001.