Voltage-gated sodium channel expression in rat and human epidermal keratinocytes: Evidence for a role in pain

Zhao, Peng; Barr, Travis P.; Hou, Quanzhi; Dib‐Hajj, Sulayman D.; Black, Joel A.; Albrecht, Phillip J.; Petersen, Karin L.; Eisenberg, Elon; Wymer, James P.; Rice, Frank L.; Waxman, Stephen G.

doi:10.1016/j.pain.2008.03.016

Cited by 161 publications

(183 citation statements)

References 56 publications

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“…The only drugs known to interact with Nav1.2 are the anticonvulsants. Nav1.2 is expressed on keratinocytes and appears to be associated with pain [49]. Carbamazepine and phenytoin bind the same site on Nav1.2.…”

Section: Results: Disproportionate Molecular Targets Identified By Damentioning

confidence: 99%

Data Mining FAERS to Analyze Molecular Targets of Drugs Highly Associated with Stevens-Johnson Syndrome

Burkhart

Abernethy

Jackson³

2015

J. Med. Toxicol.

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Drug features that are associated with StevensJohnson syndrome (SJS) have not been fully characterized. A molecular target analysis of the drugs associated with SJS in the FDA Adverse Event Reporting System (FAERS) may contribute to mechanistic insights into SJS pathophysiology. The publicly available version of FAERS was analyzed to identify disproportionality among the molecular targets, metabolizing enzymes, and transporters for drugs associated with SJS. The FAERS in-house version was also analyzed for an internal comparison of the drugs most highly associated with SJS. Cyclooxygenases 1 and 2, carbonic anhydrase 2, and sodium channel 2 alpha were identified as disproportionately associated with SJS. Cytochrome P450 (CYPs) 3A4 and 2C9 are disproportionately represented as metabolizing enzymes of the drugs associated with SJS adverse event reports. Multidrug resistance protein 1 (MRP-1), organic anion transporter 1 (OAT1), and PEPT2 were also identified and are highly associated with the transport of these drugs. A detailed review of the molecular targets identifies important roles for these targets in immune response. The association with CYP metabolizing enzymes suggests that reactive metabolites and oxidative stress may have a contributory role. Drug transporters may enhance intracellular tissue concentrations and also have vital physiologic roles that impact keratinocyte proliferation and survival. Data mining FAERS may be used to hypothesize mechanisms for adverse drug events by identifying molecular targets that are highly associated with druginduced adverse events. The information gained may contribute to systems biology disease models.

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Section: Results: Disproportionate Molecular Targets Identified By Damentioning

confidence: 99%

Data Mining FAERS to Analyze Molecular Targets of Drugs Highly Associated with Stevens-Johnson Syndrome

Burkhart

Abernethy

Jackson³

2015

J. Med. Toxicol.

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“…This might be important in CRPS. For instance, Zhao et al (Zhao et al, 2008) reported that sodium channel expression was increased in the keratinocyte layer of patients with CRPS and post herpetic neuralgia, and the beta-isoform of the inflammatory neuropeptide CGRP was found to be increased in keratinocytes both in CRPS patients and in animal models of pain (Hou et al, 2011).…”

Section: Accepted M Manuscriptmentioning

confidence: 99%

Inflammation in CRPS: Role of the sympathetic supply

Schlereth

Drummond

Birklein

2014

Autonomic Neuroscience

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Acute Complex regional Pain Syndrome (CRPS) is associated with signs of inflammation such as increased skin temperature, edema, skin colour changes and pain. Pro-inflammatory cytokines (tumor necrosis factor-α (TNF-α), interleukin-2 (IL-2), IL-1beta, IL-6) are up-regulated, whereas anti-inflammatory cytokines (IL-4, IL-10) are diminished. Adaptive immunity seems to be involved in CRPS pathophysiology as many patients have autoantibodies directed against β 2 adrenergic and muscarinic-2 receptors. In an animal tibial fracture model changes in the innate immune response such as up-regulation of keratinocytes are also found. Additionally, CRPS is accompanied by increased neurogenic inflammation which depends mainly on neuropeptides such as CGRP and Substance P.Besides inflammatory signs, sympathetic nervous system involvement in CRPS results in cool skin, increased sweating and sympathetically-maintained pain. The norepinephrine level is lower in the CRPS-affected than contralateral limb, but sympathetic sprouting and up-regulation of alphaadrenoceptors may result in an adrenergic supersensitivity.The sympathetic nervous system and inflammation interact: norepinephrine influences the immune system and the production of cytokines. There is substantial evidence that this interaction contributes to the pathophysiology and clinical presentation of CRPS, but this interaction is not straightforward. How inflammation in CRPS might be exaggerated by sympathetic transmitters requires further elucidation.

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“…Sadly enough only fragmentary insight exists in the role and the peripheral expression of sodium channels in pain-transducing free nerve ending in the skin and on the keratinocytes [28]. The sodium channels, Nav1.1, Nav1.6 and Nav1.8 are abundantly present at epidermal keratinocytes [29]. These sodium channel have differential patterns of distribution within the epidermis.…”

Section: Voltage-gated Sodium Channels: a Key Target For Phenytoinmentioning

confidence: 99%

“…Labeled axons within the dermis were detected for Nav1.2, Nav1.7, Nav1.8 and Nav1.9, but its immunolabeling was much less intense compared to the keratinocytes. It was suggested that these channels could possibly contribute to pain [29]. Pathological increases have been documented in keratinocyte sodium channel expression found in skin biopsies of patients suffering from neuropathic pain [29].…”

Section: Voltage-gated Sodium Channels: a Key Target For Phenytoinmentioning

confidence: 99%

Topical Phenytoin in Neuralgic Pain, Peripheral Modulation of Central Sensitization: Two Case Reports

Hesselink¹,

Kopsky²

2017

J Pain Relief

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We herewith describe a topical formulation of phenytoin with a clear analgesic effect in localized neuropathic pain: in post herpetic neuralgia and trigeminal neuralgia. Such topical analgesic effect for phenytoin has not yet been described in literature. We have developed various topical phenytoin formulations and identified a stable cream base in which we compounded a range of concentrations of phenytoin up to 10%. We will present two cases supporting the analgesic effect of phenytoin cream in neuralgic pain, and discuss the putative mechanism of action of phenytoin as a topical analgesic. The essence of both cases is that, apparently, it is possible to down-regulate central sensitization processes via the modulation (inhibition) of peripheral input. This hypothesis was brought forward in 2013 based on neurophysiological data, and our clinical data seem to also support this important chapter in pain treatment. Thus, topical analgesia, in our case based on phenytoin, can play an important role in multimodal therapy of chronic neuropathic pain, related to central sensitization states.

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Voltage-gated sodium channel expression in rat and human epidermal keratinocytes: Evidence for a role in pain

Cited by 161 publications

References 56 publications

Data Mining FAERS to Analyze Molecular Targets of Drugs Highly Associated with Stevens-Johnson Syndrome

Data Mining FAERS to Analyze Molecular Targets of Drugs Highly Associated with Stevens-Johnson Syndrome

Inflammation in CRPS: Role of the sympathetic supply

Topical Phenytoin in Neuralgic Pain, Peripheral Modulation of Central Sensitization: Two Case Reports

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