Sodium Channel Expression and Localization at Demyelinated Sites in Painful Human Dental Pulp

Henry, Michael; Luo, Songjiang; Foley, B.D.; Rzasa, Rachael S.; Johnson, Luke A.; Levinson, S. Rock

doi:10.1016/j.jpain.2009.01.264

Cited by 36 publications

(45 citation statements)

References 33 publications

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“…This antibody has been widely used in previous studies to identify NaCh clusters at nodes of Ranvier in both CNS and PNS and the staining pattern seen in the current study is consistent with other studies [16,39,40,72]. …”

Section: Methodssupporting

confidence: 91%

“…Results from these studies consistently showed a prominent demyelinating response of axons within the pulpitis samples that resulted in the increased incidence of atypical nodal forms. Our study with the pan-specific NaCh antibody included a quantification of NaCh clusters that lacked caspr and our results showed these "naked" NaCh accumulations were present in both normal and painful specimens [16]. Even though some of these "naked" clusters most likely result from the loss of myelin, their common occurrence in normal specimens as seen in our pan-specific NaCh study and the findings presented here provide additional evidence for their existence in unmyelinated fibers.…”

Section: Discussionsupporting

confidence: 60%

“…Results from these studies have included the identification of NaCh clusters at non-nodal sites in both normal and diseased/painful samples [16]. In this study we take the opportunity to characterize the fibers with NaCh accumulations at non-nodal sites to test the hypothesis that the unmyelinated segments of myelinated axons show an inherent ability to cluster NaChs.…”

Section: Introductionmentioning

confidence: 99%

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Unmyelinated nerve fibers in the human dental pulp express markers for myelinated fibers and show sodium channel accumulations

2012

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Background The dental pulp is a common source of pain and is used to study peripheral inflammatory pain mechanisms. Results show most fibers are unmyelinated, yet recent findings in experimental animals suggest many pulpal afferents originate from fibers that are myelinated at more proximal locations. Here we use the human dental pulp and confocal microscopy to examine the staining relationships of neurofilament heavy (NFH), a protein commonly expressed in myelinated afferents, with other markers to test the possibility that unmyelinated pulpal afferents originate from myelinated axons. Other staining relationships studied included myelin basic protein (MBP), protein gene product (PGP) 9.5 to identify all nerve fibers, tyrosine hydroxylase (TH) to identify sympathetic fibers, contactin-associated protein (caspr) to identify nodal sites, S-100 to identify Schwann cells and sodium channels (NaChs). Results Results show NFH expression in most PGP9.5 fibers except those with TH and include the broad expression of NFH in axons lacking MBP. Fibers with NFH and MBP show NaCh clusters at nodal sites as expected, but surprisingly, NaCh accumulations are also seen in unmyelinated fibers with NFH, and in fibers with NFH that lack Schwann cell associations. Conclusions The expression of NFH in most axons suggests a myelinated origin for many pulpal afferents, while the presence of NaCh clusters in unmyelinated fibers suggests an inherent capacity for the unmyelinated segments of myelinated fibers to form NaCh accumulations. These findings have broad implications on the use of dental pulp to study pain mechanisms and suggest possible novel mechanisms responsible for NaCh cluster formation and neuronal excitability.

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Section: Methodssupporting

confidence: 91%

Section: Discussionsupporting

confidence: 60%

Section: Introductionmentioning

confidence: 99%

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Unmyelinated nerve fibers in the human dental pulp express markers for myelinated fibers and show sodium channel accumulations

2012

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“…Because myelin domains define both cytoarchitecture and molecular signature of A-afferents, demyelination causes electrical instability, ectopic insertion of ion channels, and ultimately, mechanical pain hypersensitivity [2, 5, 41, 42]. In addition to MMP-mediated demyelination, MMPs may regulate the pathogenesis of mechanical allodynia [4] via control of the structural and molecular assembly of myelinated axons.…”

Section: Discussionmentioning

confidence: 99%

“…In myelin gaps (nodes of Ranvier), voltage-gated sodium channel clustering warrants rapid, saltatory conduction [3]. Demyelination of A-afferents contributes to the pathogenesis of mechanical pain hypersensitivity via disruption in this precise molecular and structural signature, including ectopic insertion of ion channels [2, 4, 5]. Among such myelin-related changes contributing to mechanical allodynia we proposed is liberation of myelin auto-antigens, such as myelin basic protein (MBP), leading to the formation of the algesic complexes on A-afferents [6–8].…”

Section: Introductionmentioning

confidence: 99%

Reciprocal relationship between membrane type 1 matrix metalloproteinase and the algesic peptides of myelin basic protein contributes to chronic neuropathic pain

Hong

Remacle

Shiryaev

et al. 2017

Brain, Behavior, and Immunity

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Myelin basic protein (MBP) is an auto-antigen able to induce intractable pain from innocuous mechanical stimulation (mechanical allodynia). The mechanisms provoking this algesic MBP activity remain obscure. Our present study demonstrates that membrane type 1 matrix metalloproteinase (MT1-MMP/MMP-14) releases the algesic MBP peptides from the damaged myelin, which then reciprocally enhance the expression of MT1-MMP in nerve to sustain a state of allodynia. Specifically, MT1-MMP expression and activity in rat sciatic nerve gradually increased starting at day 3 after chronic constriction injury (CCI). Inhibition of the MT1-MMP activity by intraneural injection of the function-blocking human DX2400 monoclonal antibody at day 3 post-CCI reduced mechanical allodynia and neuropathological signs of Wallerian degeneration, including axon demyelination, degeneration, edema and formation of myelin ovoids. Consistent with its role in allodynia, the MT1-MMP proteolysis of MBP generated the MBP69-86-containing epitope sequences in vitro. In agreement, the DX2400 therapy reduced the release of the MBP69-86 epitope in CCI nerve. Finally, intraneural injection of the algesic MBP69-86 and control MBP2-18 peptides differentially induced MT1-MMP and MMP-2 expression in the nerve. With these data we offer a novel, self-sustaining mechanism of persistent allodynia via the positive feedback loop between MT1-MMP and the algesic MBP peptides. Accordingly, short-term inhibition of MT1-MMP activity presents a feasible pharmacological approach to intervene in this molecular circuit and the development of neuropathic pain.

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The role of sodium channels in chronic pain

2012

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Here we review recent research into the mechanisms of chronic pain that has focused on neuronal sodium channels, a target of classic analgesic agents. We first discuss evidence that specific sodium channel isoforms are essential for the detection and conduction of normal acutely painful stimuli from nociceptors. We then review findings that show changes in sodium channel expression and localization in chronic inflammation and nerve injury in animal and human tissues. We conclude by discussing the role that myelination plays in organizing and maintaining sodium channel clusters at nodes of Ranvier in normal development and how inflammatory processes or nerve injury alter the characteristics of such clusters. Based on these findings, we suggest that chronic pain may in part result from partial demyelination of axons during chronic injury, which creates aberrant sodium channel clusters that serve as sites of ectopic sensitivity or spontaneous activity.

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Sodium Channel Expression and Localization at Demyelinated Sites in Painful Human Dental Pulp

Cited by 36 publications

References 33 publications

Unmyelinated nerve fibers in the human dental pulp express markers for myelinated fibers and show sodium channel accumulations

Unmyelinated nerve fibers in the human dental pulp express markers for myelinated fibers and show sodium channel accumulations

Reciprocal relationship between membrane type 1 matrix metalloproteinase and the algesic peptides of myelin basic protein contributes to chronic neuropathic pain

The role of sodium channels in chronic pain

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