Modulation of paratrigeminal nociceptive neurons following temporomandibular joint inflammation in rats

Yamazaki, Yoshio; Ren, Ke; Shimada, Masahiko; Iwata, Koichi

doi:10.1016/j.expneurol.2008.08.005

Cited by 40 publications

(25 citation statements)

References 46 publications

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“…Similar to the response at caudal Vc, TMJ-evoked Fos-LI at the dPa5 increased with greater stimulus intensity, was mainly ipsilateral to the stimulus and was enhanced by high estrogen conditions (Bereiter 2001; Okamoto et al 2008). Lesion of the dPa5 prevented cardiovascular reflex responses to noxious stimuli (Yu et al 2002), while recording studies found that dPa5 neurons encoded facial skin stimulus intensity and became sensitized after TMJ injury (Yamazaki et al 2008). Although the dPa5 likely is critical for somatic autonomic integration in the trigeminal system (Saxon and Hopkins 1998; Caous et al 2001), these studies were performed in male animals, and thus, it is not known if sex differences influence the contribution of dPa5 to TMJ nociceptive processing.…”

Section: Discussionmentioning

confidence: 99%

“…C-fos immunohistochemical studies have confirmed that select regions of the TBNC that receive direct input from the TMJ, e.g., dorsal paratrigeminal region (dPa5) and superficial laminae of Vc and upper cervical dorsal horn (C 1–2 ), encode the intensity of an intra-TMJ stimulus in an estrogen-dependent manner (Bereiter 2001; Okamoto et al 2008). Anatomical tract-tracing combined with c-fos methods have been used to report that TBNC neurons responsive to jaw muscle (Ikeda et al 2003; Sugiyo et al 2005) or TMJ injury (Yamazaki et al 2008) projected to higher brain centers associated with nociceptive processing; however, only male animals were included in these studies.…”

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confidence: 99%

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Differential ascending projections of temporomandibular joint-responsive brainstem neurons to periaqueductal gray and posterior thalamus of male and female rats

2012

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Several craniofacial pain conditions including temporomandibular joint disorders (TMJD) are more prevalent in women than men. The basis for sex differences in deep craniofacial pain is not known. The present study compared the magnitude of ascending projections from TMJ-responsive neurons in trigeminal brainstem to the ventrolateral periaqueductal gray (vlPAG) or posterior nucleus of the thalamus (Po) in males and female rats. Fluorogold (FG) was injected into vlPAG or Po and TMJ-responsive neurons were identified by Fos-like immunoreactivity (Fos-LI) after mustard oil injection. TMJ-evoked Fos-LI was similar in males and females; however, significant differences in cell counts were seen for FG single-labeled and Fos/FG double-labeled neurons in trigeminal brainstem. After vlPAG injections, the number of FG-labeled neurons in trigeminal subnucleus interpolaris (Vi), ventral interpolaris/caudalis transition (vl-Vi/Vc) and dorsal paratrigeminal region (dPa5) was greater in females than males. The percentage of Fos/FG double-labeled neurons in vl-Vi/Vc and dPa5 after vlPAG injection also were greater in females than males. By contrast after Po injections, males displayed a greater number of FG-labeled neurons in superficial laminae of Vc and C1–2 and deeper laminae at C1–2 than females. The percentage of Fos/FG double-labeled neurons in superficial laminae of Vc after Po injection also was greater in males than females. These data revealed significant sex differences in ascending projections from TMJ-responsive neurons in trigeminal brainstem. Such differences may influence the ability of males and females to recruit autonomic reflexes and endogenous pain control circuits relevant for TMJ nociception.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

Differential ascending projections of temporomandibular joint-responsive brainstem neurons to periaqueductal gray and posterior thalamus of male and female rats

2012

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“…Despite observing similar TMJ-evoked responses of units in naïve and CFA-treated rats prior to PD98059 application, the effectiveness of PD98059 on TMJ unit activity was markedly enhanced 2 weeks after CFA. Although testing at 2 weeks after intra-TMJ injection of CFA has confirmed ongoing behavioral hyperalgesia (Yamazaki et al, 2008), the exact role of TMJ units in superficial laminae at the Vc/C 1–2 region in mediating changes in behavior is not yet known. Others have claimed that elevated E2 has an antihyperalgesic or even analgesic effect on TMJ-related behavior (Fischer et al, 2008; Kramer and Bellinger, 2009).…”

Section: Discussionmentioning

confidence: 99%

“…Intra-articular administration of Complete Freund’s Adjuvant (CFA) is a well-established animal model for monoarthritis that causes persistent joint inflammation (Wilson et al 2006) and long-term changes nociceptive behavior in rodents (Butler et al 1992; Schadrack et al 1999; Luo et al 2008). In male rats intra-TMJ injection of CFA produces orofacial cutaneous hyperalgesia lasting at least 2 weeks (Imbe et al, 2001; Okamoto et al, 2005a; Yamazaki et al, 2008) and increases the expression of pERK-positive neurons in Vc after jaw movement at that time (Suzuki et al, 2007). In cycling female rats, we found that 2 weeks after CFA treatment the number of Fos-positive neurons produced at the Vc/C 1–2 region after TMJ stimulation was enhanced in proestrous (high E2) compared to diestrous (low E2) female rats suggesting a role for sex hormone status in TMJ-evoked responses during chronic inflammation (Bereiter et al, 2005b).…”

Section: Introductionmentioning

confidence: 99%

Chronic inflammation and estradiol interact through MAPK activation to affect TMJ nociceptive processing by trigeminal caudalis neurons

2009

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The mitogen-activated protein kinase/extracellular regulated kinase (MAPK/ERK) pathway plays a key role in mediating estrogen actions in the brain and neuronal sensitization during inflammation. Estrogen status is a risk factor in chronic temporomandibular muscle/joint disorders (TMJD); however, the basis for this relationship is not known. The present study tested the hypothesis that estrogen status acts through the MAPK/ERK signaling pathway to alter TMJ nociceptive processing. Single TMJ-responsive neurons were recorded in laminae I–II at the spinomedullary (Vc/C1–2) junction in naïve ovariectomized (OvX) female rats treated for 2 days with high (20 μg/day; HE2) or low dose estradiol (2 μg/day; LE2) and after chronic inflammation of the TMJ region by Complete Freund’s Adjuvant (CFA) for 12–14 days. Intra-TMJ injection of ATP (1 mM) was used to activate Vc/C1–2 neurons. The MAPK/ERK inhibitor (PD98059, 0.01–1 mM) was applied topically to the dorsal Vc/C1–2 surface at the site of recording 10 min prior to each ATP stimulus. In naive HE2 rats, low dose PD98059 caused a maximal inhibition of ATP-evoked activity, whereas even high doses had only minor effects on units in LE2 rats. By contrast, after chronic TMJ inflammation, PD98059 produced a marked and similar dose-related inhibition of ATP-evoked activity in HE2 and LE2 rats. These results suggested that E2 status and chronic inflammation acted, at least in part, through a common MAPK/ERK-dependent signaling pathway to enhance TMJ nociceptive processing by laminae I–II neurons at the spinomedullary junction region.

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“…In the present study, NADPH-d stained neurons were mainly concentrated in the Vc, Pa5 and DMSp5. Pa5 are thought to be involved in processing trigeminal nociceptive information (Yamazaki et al 2008).…”

Section: Discussionmentioning

confidence: 99%

Distribution of heme oxygenase-2 and NADPH-diaphorase in the spinal trigeminal nucleus of the rat

et al. 2009

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Heme oxygenase (HO)/carbon monoxide (CO) and nitric oxide synthase (NOS)/nitric oxide (NO) systems are involved in sensory information processing. The present study was undertaken to examine the distribution of HO-2 and NOS in the spinal trigeminal nucleus (STN) of the rat, using histochemistry and immunohistochemistry. Nicotinamide adenine dinucleotide phosphate-diaphorase (NADPH-d) staining was found that NADPH-d activity was more prominent in the nucleus caudalis (Vc) and the dorsomedial subdivision of the nucleus oralis (Vo) than in other spinal trigeminal regions. Immunohistochemistry for HO-2 revealed that HO-2 staining neurons distributed extensively, which intensity was higher in the rostral than caudal part of the STN. The colocalization of NADPH-d and HO-2 was mainly confined in the Vc. The expression and distribution of NADPH-d and HO-2 suggest that NO and CO are likely neurotransmitters and might function in the processing orofacial signal in the STN together.

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Modulation of paratrigeminal nociceptive neurons following temporomandibular joint inflammation in rats

Cited by 40 publications

References 46 publications

Differential ascending projections of temporomandibular joint-responsive brainstem neurons to periaqueductal gray and posterior thalamus of male and female rats

Differential ascending projections of temporomandibular joint-responsive brainstem neurons to periaqueductal gray and posterior thalamus of male and female rats

Chronic inflammation and estradiol interact through MAPK activation to affect TMJ nociceptive processing by trigeminal caudalis neurons

Distribution of heme oxygenase-2 and NADPH-diaphorase in the spinal trigeminal nucleus of the rat

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