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Chen, K. SCN9A Gene. Encyclopedia. Available online: https://encyclopedia.pub/entry/4852 (accessed on 27 December 2024).
Chen K. SCN9A Gene. Encyclopedia. Available at: https://encyclopedia.pub/entry/4852. Accessed December 27, 2024.
Chen, Karina. "SCN9A Gene" Encyclopedia, https://encyclopedia.pub/entry/4852 (accessed December 27, 2024).
Chen, K. (2020, December 24). SCN9A Gene. In Encyclopedia. https://encyclopedia.pub/entry/4852
Chen, Karina. "SCN9A Gene." Encyclopedia. Web. 24 December, 2020.
SCN9A Gene
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This entry is adapted from the peer-reviewed paper https://medlineplus.gov/genetics/gene/scn9a

sodium voltage-gated channel alpha subunit 9

genes

1. Normal Function

The SCN9A gene belongs to a family of genes that provide instructions for making sodium channels. These channels, which transport positively charged sodium atoms (sodium ions) into cells, play a key role in a cell's ability to generate and transmit electrical signals.

The SCN9A gene provides instructions for making one part (the alpha subunit) of a sodium channel called NaV1.7. NaV1.7 sodium channels are found in nerve cells called nociceptors that transmit pain signals. Nociceptors are part of the peripheral nervous system, which connects the brain and spinal cord to cells that detect sensations such as touch, smell, and pain. Nociceptors are primarily involved in transmitting pain signals. The centers of nociceptors, known as the cell bodies, are located in a part of the spinal cord called the dorsal root ganglion. Fibers called axons extend from the cell bodies, reaching throughout the body to receive sensory information. Axons transmit the information back to the dorsal root ganglion, which then sends it to the brain. NaV1.7 sodium channels are also found in olfactory sensory neurons, which are nerve cells in the nasal cavity that transmit smell-related signals to the brain.

2. Health Conditions Related to Genetic Changes

2.1. Congenital insensitivity to pain

At least 13 mutations in the SCN9A gene have been found to cause congenital insensitivity to pain, a condition that inhibits the ability to perceive physical pain. The SCN9A gene mutations that cause congenital insensitivity to pain create a premature stop signal in the instructions for making the alpha subunit of the NaV1.7 sodium channel. As a result, a shortened, nonfunctional subunit is produced which cannot be incorporated into the channel, leading to a loss of functional NaV1.7 sodium channels. The loss of these channels impairs the transmission of pain signals from the site of injury to the brain, causing those affected to be insensitive to pain. Loss of this channel in olfactory sensory neurons likely impairs the transmission of smell-related signals to the brain, leading to a complete loss of the sense of smell (anosmia).

2.2. Erythromelalgia

More than 10 mutations in the SCN9A gene have been found to cause erythromelalgia, a condition characterized by episodes of pain, redness, and swelling in various parts of the body, particularly the hands and feet. All identified mutations change one protein building block (amino acid) in the NaV1.7 sodium channel. These mutations result in a NaV1.7 sodium channel that opens more easily than usual and stays open longer than normal, increasing the flow of sodium ions that produce nerve impulses within nociceptors. This increase in sodium ions enhances transmission of pain signals, leading to the signs and symptoms of erythromelalgia.

2.3. Paroxysmal extreme pain disorder

Approximately 10 mutations in the SCN9A gene have been found to cause paroxysmal extreme pain disorder. This condition is characterized by severe pain attacks accompanied by skin redness and warmth (flushing) and, sometimes, seizures and changes in breathing and heart rate. The mutations that cause this condition change single amino acids in the alpha subunit of the NaV1.7 sodium channel. As a result, the sodium channel does not completely close when it is turned off, allowing sodium ions to flow abnormally into nociceptors. This increase in sodium ions enhances transmission of pain signals, leading to the pain attacks experienced by people with paroxysmal extreme pain disorder.

2.4. Small fiber neuropathy

Mutations in the SCN9A gene account for approximately 30 percent of cases of small fiber neuropathy, a condition characterized by severe pain attacks and a reduced ability to differentiate between hot and cold. The mutations that cause this condition change single amino acids in the alpha subunit of the NaV1.7 sodium channel. As a result of the altered alpha subunit, the sodium channel does not completely close when it is turned off, allowing sodium ions to flow abnormally into nociceptors. This increase in sodium ions enhances transmission of pain signals. In this condition, the small fibers that extend from the nociceptors and transmit pain signals (axons) degenerate over time. The cause of this degeneration is unknown, but it likely accounts for signs and symptoms such as the loss of temperature differentiation.

2.5. Other disorders

At least three mutations in the SCN9A gene have been found in a group of people affected with febrile seizures, which are seizures that are triggered by a high fever. Febrile seizures are the most common type of seizures in young children, affecting 2 to 5 percent of children in Europe and North America. Children who have febrile seizures have a 2 to 9 percent chance of developing non-fever-related seizures later in life. When febrile seizures are associated with mutations in the SCN9A gene, the condition is known as familial febrile seizures 3B. If these individuals go on to develop seizures without fevers, the condition is then known as generalized epilepsy with febrile seizures plus, type 7. The mutations that cause these conditions change single amino acids in the alpha subunit of the NaV1.7 sodium channel. It is unknown how a change in the sodium channel leads to febrile seizures.

Variants in the SCN9A gene, when coupled with mutations in another gene called SCN1A, alter the progression of a seizure disorder called Dravet syndrome in some individuals. Dravet syndrome is characterized by convulsive seizures in infancy, followed in childhood by absence seizures, which cause loss of consciousness for short periods. In mid-childhood, the seizures change to the generalized tonic-clonic type, which involve muscle rigidity, convulsions, and loss of consciousness. Generalized tonic-clonic seizures are also associated with prolonged episodes of seizure activity known as nonconvulsive status epilepticus. These episodes can cause confusion and a loss of alertness lasting from hours to weeks. SCN1A gene mutations are the most common cause of Dravet syndrome, but when an affected individual also has a SCN9A gene change, which might not otherwise cause health problems, the signs and symptoms of Dravet syndrome are more severe. For example, individuals with both SCN1A and SCN9A gene changes may have status epilepticus in infancy and experience a variety of seizures at any time. It is unknown how SCN9A gene changes contribute to the signs and symptoms of Dravet syndrome.

3. Other Names for This Gene

  • hNE
  • Nav1.7
  • NE-NA
  • NENA
  • PN1
  • SCN9A_HUMAN
  • sodium channel, voltage gated, type IX alpha subunit
  • sodium channel, voltage-gated, type IX, alpha
  • sodium channel, voltage-gated, type IX, alpha polypeptide
  • sodium channel, voltage-gated, type IX, alpha subunit
  • voltage-gated sodium channel alpha subunit Nav1.7

References

  1. Cox JJ, Reimann F, Nicholas AK, Thornton G, Roberts E, Springell K, Karbani G,Jafri H, Mannan J, Raashid Y, Al-Gazali L, Hamamy H, Valente EM, Gorman S,Williams R, McHale DP, Wood JN, Gribble FM, Woods CG. An SCN9A channelopathycauses congenital inability to experience pain. Nature. 2006 Dec14;444(7121):894-8.
  2. Dib-Hajj SD, Cummins TR, Black JA, Waxman SG. From genes to pain: Na v 1.7 andhuman pain disorders. Trends Neurosci. 2007 Nov;30(11):555-63.Review.
  3. Dib-Hajj SD, Yang Y, Waxman SG. Genetics and molecular pathophysiology ofNa(v)1.7-related pain syndromes. Adv Genet. 2008;63:85-110. doi:10.1016/S0065-2660(08)01004-3. Review.
  4. Doty CN. SCN9A: another sodium channel excited to play a role in humanepilepsies. Clin Genet. 2010 Apr;77(4):326-8. doi:10.1111/j.1399-0004.2009.01366_1.x.
  5. Drenth JP, Waxman SG. Mutations in sodium-channel gene SCN9A cause a spectrum of human genetic pain disorders. J Clin Invest. 2007 Dec;117(12):3603-9. Review.
  6. Faber CG, Hoeijmakers JG, Ahn HS, Cheng X, Han C, Choi JS, Estacion M, Lauria G, Vanhoutte EK, Gerrits MM, Dib-Hajj S, Drenth JP, Waxman SG, Merkies IS. Gainof function Naν1.7 mutations in idiopathic small fiber neuropathy. Ann Neurol.2012 Jan;71(1):26-39. doi: 10.1002/ana.22485.
  7. Fertleman CR, Ferrie CD, Aicardi J, Bednarek NA, Eeg-Olofsson O, Elmslie FV,Griesemer DA, Goutières F, Kirkpatrick M, Malmros IN, Pollitzer M, Rossiter M,Roulet-Perez E, Schubert R, Smith VV, Testard H, Wong V, Stephenson JB.Paroxysmal extreme pain disorder (previously familial rectal pain syndrome).Neurology. 2007 Aug 7;69(6):586-95.
  8. Fischer TZ, Waxman SG. Familial pain syndromes from mutations of the NaV1.7sodium channel. Ann N Y Acad Sci. 2010 Jan;1184:196-207. doi:10.1111/j.1749-6632.2009.05110.x. Review.
  9. Goldberg YP, MacFarlane J, MacDonald ML, Thompson J, Dube MP, Mattice M,Fraser R, Young C, Hossain S, Pape T, Payne B, Radomski C, Donaldson G, Ives E,Cox J, Younghusband HB, Green R, Duff A, Boltshauser E, Grinspan GA, Dimon JH,Sibley BG, Andria G, Toscano E, Kerdraon J, Bowsher D, Pimstone SN, Samuels ME,Sherrington R, Hayden MR. Loss-of-function mutations in the Nav1.7 gene underlie congenital indifference to pain in multiple human populations. Clin Genet. 2007Apr;71(4):311-9.
  10. Hoeijmakers JG, Merkies IS, Gerrits MM, Waxman SG, Faber CG. Genetic aspectsof sodium channelopathy in small fiber neuropathy. Clin Genet. 2012Oct;82(4):351-8. doi: 10.1111/j.1399-0004.2012.01937.x.
  11. Houlden H. Extending the clinical spectrum of pain channelopathies. Brain.2012 Feb;135(Pt 2):313-6. doi: 10.1093/brain/aws007.
  12. Lampert A, O'Reilly AO, Reeh P, Leffler A. Sodium channelopathies and pain.Pflugers Arch. 2010 Jul;460(2):249-63. doi: 10.1007/s00424-009-0779-3.
  13. Meisler MH, O'Brien JE, Sharkey LM. Sodium channel gene family: epilepsymutations, gene interactions and modifier effects. J Physiol. 2010 Jun 1;588(Pt11):1841-8. doi: 10.1113/jphysiol.2010.188482.
  14. Singh NA, Pappas C, Dahle EJ, Claes LR, Pruess TH, De Jonghe P, Thompson J,Dixon M, Gurnett C, Peiffer A, White HS, Filloux F, Leppert MF. A role of SCN9Ain human epilepsies, as a cause of febrile seizures and as a potential modifierof Dravet syndrome. PLoS Genet. 2009 Sep;5(9):e1000649. doi:10.1371/journal.pgen.1000649.
  15. Waxman SG. Neurobiology: a channel sets the gain on pain. Nature. 2006 Dec14;444(7121):831-2.
  16. Waxman SG. Neuroscience: Channelopathies have many faces. Nature. 2011 Apr14;472(7342):173-4. doi: 10.1038/472173a.
  17. Young FB. When adaptive processes go awry: gain-of-function in SCN9A. ClinGenet. 2008 Jan;73(1):34-6.
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Subjects: Genetics & Heredity
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Karina Chen
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Update Date: 24 Dec 2020
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