Trigeminal transition zone/rostral ventromedial medulla connections and facilitation of orofacial hyperalgesia after masseter inflammation in rats

Sugiyo, Shinichi; Takemura, Motohide; Dubner, Ronald; Ren, Ke

doi:10.1002/cne.20797

Cited by 77 publications

(97 citation statements)

References 63 publications

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“…Furthermore, the number of nociceptive neurons that can be analyzed in single-neuron recording studies is limited in any one animal. It is probable that these fiber differences and technical limitation in single-neuron recording may be involved in the distribu- Generally, we observed a pattern of organization of pERK-LI cell expression following capsaicin stimulation of the face that was similar to that reported in previous c-Fos studies Zhou et al, 1999;Takemura et al, 2000;Watanabe et al, 2002;Nomura et al, 2002;Bereiter et al, 2005;Sato et al, 2005;Sugiyo et al, 2005Sugiyo et al, , 2006. However, the distribution of pERK-LI cells was more restricted from the Vi/Vc zone through the Vc/C2 zone compared with previous reports of c-Fospositive neurons Mineta et al, 1995).…”

Section: Dorsoventral and Rostrocaudal Organization Of Perk-li Cellssupporting

confidence: 81%

“…Another approach that has been used is c-Fos labeling to delineate the arrangement of nociceptive neurons in the trigeminal spinal nucleus and upper cervical cord as well as spinal dorsal horn. After noxious stimulation of a variety of orofacial sites, Fos protein like-immunoreactive cells (Fos-LI cells) occur in the trigeminal spinal nucleus interpolaris (Vi) and caudalis (Vc) transition zone (Vi/Vc zone) and the Vc/C2 transition zone Iwata et al, 1998a;Zhou et al, 1999;Takemura et al, 2000;Nomura et al, 2002;Watanabe et al, 2002;Kawabata et al, 2004;Bereiter et al, 2005;Sato et al, 2005;Sugiyo et al, 2005Sugiyo et al, , 2006Shimizu et al, 2006) in a somatotopic arrangement, and their numbers increase as noxious stimulus intensity increases Mineta et al, 1995). However, it has been reported that the c-Fos expression starts at about 30 minutes and peaks about 1 hour after noxious stimulation (Hunt et al, 1987;Tokunaga et al, 1995) in both superficial and deep laminae of the spinal dorsal horn (DH; Bullitt, 1991), so it is very likely that c-Fos expression is not directly correlated with an activation of Vc and upper cervical nociceptive neurons following acute orofacial noxious stimulation.…”

Section: Indexing Terms: Somatotopic Organization; Nociceptive Neuronmentioning

confidence: 98%

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Organization of pERK‐immunoreactive cells in trigeminal spinal nucleus caudalis and upper cervical cord following capsaicin injection into oral and craniofacial regions in rats

Noma

Tsuboi

Kondo

et al. 2008

J of Comparative Neurology

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To define the somatotopic arrangement of neurons in the trigeminal spinal subnucleus caudalis and upper cervical cord activated by acute noxious stimulation of various orofacial sites, pERK expression was analyzed in these neurons. After capsaicin injection into the tongue, lower gum, upper and lower lips, or mental region, pERK-like immunoreactive (pERK-LI) cells were distributed mainly in the dorsal half of the trigeminal spinal nucleus interporalis (Vi) and caudalis (Vc) transition zone (Vi/Vc zone), middle Vc, and Vc and upper cervical cord transition zone (Vc/C2 zone). pERK-LI cells were distributed throughout the dorsal to ventral portion of the Vi/Vc zone, middle Vc, and Vc/C2 zone following capsaicin injection into the anterior hard palate, upper gum, buccal mucosa, or vibrissal pad and in the ventral portion of the Vi/Vc zone, middle Vc, and Vc/C2 zone following snout, ophthalmic, or ocular injection of capsaicin. The rostrocaudal distribution area of pERK-LI cells was more extensive from the Vi/Vc zone to the Vc/C2 zone after intraoral injection than that after facial injection, and the rostrocaudal distribution of pERK-LI cells from the Vi/Vc zone to the Vc/C2 zone had a somatotopic arrangement, with the snout being represented most rostrally and ophthalmic, ocular, or mental regions represented most caudally. These findings suggest that the pERK-LI cells expressed from the Vi/Vc zone to the Vc/C2 zone following injection of capsaicin in facial and intraoral structures may be differentially involved in pain perception in facial and intraoral sites.

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Section: Dorsoventral and Rostrocaudal Organization Of Perk-li Cellssupporting

confidence: 81%

Section: Indexing Terms: Somatotopic Organization; Nociceptive Neuronmentioning

confidence: 98%

Organization of pERK‐immunoreactive cells in trigeminal spinal nucleus caudalis and upper cervical cord following capsaicin injection into oral and craniofacial regions in rats

Noma

Tsuboi

Kondo

et al. 2008

J of Comparative Neurology

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“…Local anesthesia of RVM attenuates mustard oilinduced hyperexcitability of spinal dorsal horn neurons [16] and behavioral hyperalgesia [17]. Lesions of the RVM suppress formalin-induced nocifensive behavior [18], inhibit secondary hyperalgesia produced by topical application of mustard oil [15], and attenuate (secondary) mechanical hyperalgesia after masseter muscle inflammation induced by complete Freund's adjuvant (CFA) [19]. The same phenomenon occurs in models of neuropathic pain.…”

Section: Pain Modulatory Circuitry and Behavioral Hyperalgesiamentioning

confidence: 85%

Pain Facilitation and Activity-Dependent Plasticity in Pain Modulatory Circuitry: Role of BDNF-TrkB Signaling and NMDA Receptors

2007

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Pain modulatory circuitry in the brainstem exhibits considerable synaptic plasticity. The increased peripheral neuronal barrage after injury activates spinal projection neurons that then activate multiple chemical mediators including glutamatergic neurons at the brainstem level, leading to an increased synaptic strength and facilitatory output. It is not surprising that a well-established regulator of synaptic plasticity, brain-derived neurotrophic factor (BDNF), contributes to the mechanisms of descending pain facilitation. After tissue injury, BDNF and TrkB signaling in the brainstem circuitry is rapidly activated. Through the intracellular signaling cascade that involves phospholipase C, inositol trisphosphate, protein kinase C, and nonreceptor protein tyrosine kinases; N-methyl-D-aspartate (NMDA) receptors are phosphorylated, descending facilitatory drive is initiated, and behavioral hyperalgesia follows. The synaptic plasticity observed in the pain pathways shares much similarity with more extensively studied forms of synaptic plasticity such as long-term potentiation (LTP) and long-term depression (LTD), which typically express NMDA receptor dependency and regulation by trophic factors. However, LTP and LTD are experimental phenomena whose relationship to functional states of learning and memory has been difficult to prove. Although mechanisms of synaptic plasticity in pain pathways have typically not been related to LTP and LTD, pain pathways have an advantage as a model system for synaptic modifications as there are many well-established models of persistent pain with clear measures of the behavioral phenotype. Further studies will elucidate cellular and molecular mechanisms of pain sensitization and further our understanding of principles of central nervous system plasticity and responsiveness to environmental challenge.

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“…Following injection of the retrograde tracer Fluorogold into the Vi/Vc transition zone, retrogradely labeled cells were observed in the Vc/C1,2 region (Sato et al ., 2005). After lesions of the bilateral Vc, there is a selective reduction of inflammation-induced Fos-expressing neurons in the ventral Vi/Vc, but not in dorsal or intermediate Vi/Vc, or nucleus tractus solitarius (Sugiyo et al ., 2005). These findings support that trigeminal transition zone activity, particularly the ventral Vi/Vc, is modulated by the activation of the caudal laminated Vc zone.…”

Section: Functional Input and Output Of The Vi/vc Transition Zonementioning

confidence: 99%

The Role Of Trigeminal Interpolaris-Caudalis Transition Zone In Persistent Orofacial Pain

Ren

Dubner

2011

International Review of Neurobiology

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Trigeminal transition zone/rostral ventromedial medulla connections and facilitation of orofacial hyperalgesia after masseter inflammation in rats

Cited by 77 publications

References 63 publications

Organization of pERK‐immunoreactive cells in trigeminal spinal nucleus caudalis and upper cervical cord following capsaicin injection into oral and craniofacial regions in rats

Organization of pERK‐immunoreactive cells in trigeminal spinal nucleus caudalis and upper cervical cord following capsaicin injection into oral and craniofacial regions in rats

Pain Facilitation and Activity-Dependent Plasticity in Pain Modulatory Circuitry: Role of BDNF-TrkB Signaling and NMDA Receptors

The Role Of Trigeminal Interpolaris-Caudalis Transition Zone In Persistent Orofacial Pain

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