A sodium channel gene <i>SCN9A</i> polymorphism that increases nociceptor excitability

Estacion, Mark; Harty, T. Patrick; Choi, Jin-Sung; Tyrrell, Lynda; Dib‐Hajj, Sulayman D.; Waxman, Stephen G.

doi:10.1002/ana.21895

Cited by 90 publications

(65 citation statements)

References 21 publications

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“…By contrast, most Na v 1.7 mutations associated with hyperexcitability and erythromelalgia have been reported to shift the voltage dependence of activation in the opposite, hyperpolarizing direction (26,28). Nevertheless, Na v 1.7-1150W produced hyperexcitability when expressed in small dorsal root ganglion neurons (27), a finding that is consistent with the clinical results presented here. The exact mechanism by which the minor A allele enhances pain sensitivity therefore remains unclear and might involve factors not present in the heterologous expression system, factors that affect expression, processing, or interaction of the Na v 1.7 protein in nociceptive neurons.…”

Section: Discussionsupporting

confidence: 89%

“…However, the observed biophysical effect is rather small and might be insufficient to explain the associated phenotype, because alteration of the slow inactivation of the Na v 1.7 conductance alone in the absence of altered voltage-dependent activation failed to change the firing properties in a computer model of nociceptive neurons (26). It is important to note that another recent study failed to observe a change in voltage dependence of slow inactivation, but instead reported a small depolarizing shift in the voltage dependence of activation for Na v 1.7-1150W compared to Na v 1.7-1150R currents (27). By contrast, most Na v 1.7 mutations associated with hyperexcitability and erythromelalgia have been reported to shift the voltage dependence of activation in the opposite, hyperpolarizing direction (26,28).…”

Section: Discussionmentioning

confidence: 86%

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Pain perception is altered by a nucleotide polymorphism in SCN9A

Reimann¹,

Cox

Belfer

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

279

169

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The gene SCN9A is responsible for three human pain disorders. Nonsense mutations cause a complete absence of pain, whereas activating mutations cause severe episodic pain in paroxysmal extreme pain disorder and primary erythermalgia. This led us to investigate whether single nucleotide polymorphisms (SNPs) in SCN9A were associated with differing pain perception in the general population. We first genotyped 27 SCN9A SNPs in 578 individuals with a radiographic diagnosis of osteoarthritis and a pain score assessment. A significant association was found between pain score and SNP rs6746030; the rarer A allele was associated with increased pain scores compared to the commoner G allele (P = 0.016). This SNP was then further genotyped in 195 pain-assessed people with sciatica, 100 amputees with phantom pain, 179 individuals after lumbar discectomy, and 205 individuals with pancreatitis. The combined P value for increased A allele pain was 0.0001 in the five cohorts tested (1277 people in total). The two alleles of the SNP rs6746030 alter the coding sequence of the sodium channel Nav1.7. Each was separately transfected into HEK293 cells and electrophysiologically assessed by patch-clamping. The two alleles showed a difference in the voltagedependent slow inactivation (P = 0.042) where the A allele would be predicted to increase Nav1.7 activity. Finally, we genotyped 186 healthy females characterized by their responses to a diverse set of noxious stimuli. The A allele of rs6746030 was associated with an altered pain threshold and the effect mediated through C-fiber activation. We conclude that individuals experience differing amounts of pain, per nociceptive stimulus, on the basis of their SCN9A rs6746030 genotype.Na v 1.7 | nociception | pain | SCN9A | single nucleotide polymorphisms

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Section: Discussionsupporting

confidence: 89%

Section: Discussionmentioning

confidence: 86%

Pain perception is altered by a nucleotide polymorphism in SCN9A

Reimann¹,

Cox

Belfer

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

279

169

View full text Add to dashboard Cite

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“…Finally, the mechanism(s) whereby CACNG2 polymorphisms affect spontaneous pain can be expected to inform our understanding of pain physiology. Several pain susceptibility genes have been identified previously based on family linkage studies or candidate gene approaches, including one remarkable example in which a genetic polymorphism directly related to mechanisms that regulate the electrical excitability of DRG neurons (Estacion et al 2009). …”

Section: Discussionmentioning

confidence: 99%

Susceptibility to chronic pain following nerve injury is genetically affected by CACNG2

Nissenbaum¹,

Devor²,

Seltzer³

et al. 2010

Genome Res.

123

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Chronic neuropathic pain is affected by specifics of the precipitating neural pathology, psychosocial factors, and by genetic predisposition. Little is known about the identity of predisposing genes. Using an integrative approach, we discovered that CACNG2 significantly affects susceptibility to chronic pain following nerve injury. CACNG2 encodes for stargazin, a protein intimately involved in the trafficking of glutamatergic AMPA receptors. The protein might also be a Ca 2+ channel subunit. CACNG2 has previously been implicated in epilepsy. Initially, using two fine-mapping strategies in a mouse model (recombinant progeny testing [RPT] and recombinant inbred segregation test [RIST]), we mapped a painrelated quantitative trait locus (QTL) (Pain1) into a 4.2-Mb interval on chromosome 15. This interval includes 155 genes. Subsequently, bioinformatics and whole-genome microarray expression analysis were used to narrow the list of candidates and ultimately to pinpoint Cacng2 as a likely candidate. Analysis of stargazer mice, a Cacng2 hypomorphic mutant, provided electrophysiological and behavioral evidence for the gene's functional role in pain processing. Finally, we showed that human CACNG2 polymorphisms are associated with chronic pain in a cohort of cancer patients who underwent breast surgery. Our findings provide novel information on the genetic basis of neuropathic pain and new insights into pain physiology that may ultimately enable better treatments.[Supplemental material is available online at http://www.genome.org. The human data from this study have been submitted to the Human Genome Variation Database of Genotype-to-Phenotype (http://www.hgvbaseg2.org) under accession no. HGVST514.]Chronic pain is a healthcare problem of enormous proportions, directly affecting nearly 20% of adults and associated with massive financial costs (Breivik et al. 2006). At least 25% of this burden is attributable to ''neuropathic pain,'' pain that follows nerve damage (Bouhassira et al. 2008). In patients with neuropathy spontaneous pain is typically the most prominent cause of suffering, rather than stimulus-provoked pain. A striking example is phantom pain. Virtually all limb amputees report feeling a phantom limb, and most report spontaneous burning, stabbing, or electric shocklike pain, at least occasionally (Sherman et al. 1996;Nikolajsen and Jensen 2001). Phantom pain is also common after breast removal (Tytherleigh et al. 1998;Rothemund et al. 2004;Vadivelu et al. 2008) and in body parts that have been denervated but are still present (''anesthesia dolorosa'') (Wynn Parry 1980). Neuropathic pain, including phantom pain, is a complex trait affected by both the nature of the neural injury and by psychosocial factors. Its notorious variability among individuals, even when the underlying nerve pathology is identical, has prompted awareness of a significant genetic contribution to the amount of pain felt (Diatchenko et al. 2007;Lacroix-Fralish and Mogil 2008;LaCroix-Fralish et al. 2009). At present, the biological process ...

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“…To date, nine functionally distinct mammalian NaV channel alpha subunits (NaV1.1-NaV1.9) have been cloned, functionally expressed, and characterized [13]. In recent years, the tetrodotoxin-sensitive sodium channel NaV1.7 has emerged as an analgesic target and polymorphisms in the Na(V)1.7 channel may influence susceptibility to pain [14,15].…”

Section: Introductionmentioning

confidence: 99%

Evaluation of behavior and expression of NaV1.7 in dorsal root ganglia after sciatic nerve compression and application of nucleus pulposus in rats

et al. 2013

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Purpose The pathomechanisms of pain resulting from lumbar disc herniation have not been fully elucidated. Prostaglandins and cytokines generated at the inflammatory site produce associated pain; however, non-steroidal anti-inflammatory drugs and steroids are sometimes ineffective in patients. Tetrodotoxin-sensitive voltage-gated sodium (NaV) channels are related to sensory transmission in primary sensory nerves. The sodium channel NaV1.7 has emerged as an attractive analgesic target. The purpose of this study was to evaluate pain-related behavior and expression of NaV1.7 in dorsal root ganglia (DRG) after combined sciatic nerve compression and nucleus pulposus (NP) application in rats. Methods Rats were divided into three groups and underwent either sciatic nerve compression with NP for 2 s using forceps (n = 20), sham operation with neither compression nor NP (n = 20), or no operation (controls, n = 20). Mechanical hyperalgesia was measured every second day for three weeks using von Frey filaments. NaV1.7 expression in L5 DRG was examined 7 and 14 days after surgery using immunohistochemistry. The number of neurons immunoreactive for NaV1.7 was compared among the three groups. Results Mechanical hyperalgesia was found over the 14-day observation in the nerve compression plus NP application group, but not in the sham-operated or control groups (P \ 0.05). NaV1.7 expression in L5 DRG was up-regulated in the nerve compression plus NP application group, compared with sham-operated and control rats (P \ 0.01). Conclusions Our results indicate that nerve compression plus NP application produces pain-related behavior. We conclude that NaV1.7 expression in DRG neurons may play an important role in mediating pain from sciatic nerves after compression injury and exposure to NP.

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A sodium channel gene SCN9A polymorphism that increases nociceptor excitability

Cited by 90 publications

References 21 publications

Pain perception is altered by a nucleotide polymorphism in SCN9A

Pain perception is altered by a nucleotide polymorphism in SCN9A

Susceptibility to chronic pain following nerve injury is genetically affected by CACNG2

Evaluation of behavior and expression of NaV1.7 in dorsal root ganglia after sciatic nerve compression and application of nucleus pulposus in rats

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