Sodium channel

Sodium channels are integral membrane proteins that form ion channels, conducting sodium ions (Na⁺) through a cell's plasma membrane.^[1][2] They are classified according to the trigger that opens the channel for such ions, i.e. either a voltage-change (voltage-gated sodium channels) or binding of a substance (a ligand) to the channel (ligand-gated sodium channels).

In excitable cells such as neurons, myocytes, and certain types of glia, sodium channels are responsible for the rising phase of action potentials.

Voltage-gated

Structure

Diagram of a voltage-sensitive sodium channel α-subunit. G - glycosylation, P - phosphorylation, S - ion selectivity, I - inactivation, positive (+) charges in S4 are important for transmembrane voltage sensing.^[3]

Sodium channels consist of a large α subunit that associates with other proteins, such as β subunits. An α subunit forms the core of the channel and is functional on its own. When the α subunit protein is expressed by a cell, it is able to form channels that conduct Na⁺ in a voltage-gated way, even if β subunits or other known modulating proteins are not expressed. When accessory proteins assemble with α subunits, the resulting complex can display altered voltage dependence and cellular localization.

The α-subunit has four repeat domains, labeled I through IV, each containing six membrane-spanning regions, labeled S1 through S6. The highly conserved S4 region acts as the channel's voltage sensor. The voltage sensitivity of this channel is due to positive amino acids located at every third position. When stimulated by a change in transmembrane voltage, this region moves toward the extracellular side of the cell membrane, allowing the channel to become permeable to ions. The ions are conducted through a pore, which can be broken into two regions. The more external (i.e., more extracellular) portion of the pore is formed by the "P-loops" (the region between S5 and S6) of the four domains. This region is the most narrow part of the pore and is responsible for its ion selectivity. The inner portion (i.e., more cytoplasmic) of the pore is formed by the combined S5 and S6 regions of the four domains. The region linking domains III and IV is also important for channel function. This region plugs the channel after prolonged activation, inactivating it.

Gating

Voltage-gated sodium channels have three types of states: deactivated (closed), activated (open), and inactivated (closed). Channels in the deactivated state are thought to be blocked on their intracellular side by an "activation gate", which is removed in response to stimulation that opens the channel. The ability to inactivate is thought to be due to a tethered plug (formed by domains III and IV of the alpha subunit), called an inactivation gate, that blocks the inside of the channel shortly after it has been activated. During an action potential the channel remains inactivated for a few milliseconds after depolarization. The inactivation is removed when the membrane potential of the cell repolarizes following the falling phase of the action potential. This allows the channels to be activated again during the next action potential. Genetic diseases that alter sodium channel inactivation can cause muscle stiffness or epileptic seizures because of the introduction of a so-called window current, during which sodium channels are tonically active, causing muscle and/or nerve cells to become over-excited.

The temporal behaviour of sodium channels can be modeled by a Markovian scheme or by the Hodgkin-Huxley-type formalism. In the former scheme, each channel occupies a distinct state with differential equations describing transitions between states; in the latter, the channels are treated as a population that are affected by three independent gating variables. Each of these variables can attain a value between 1 (fully permeant to ions) and 0 (fully non-permeant), the product of these variables yielding the percentage of conducting channels.

Impermeability to other ions

The pore of sodium channels contains a selectivity filter made of negatively charged amino acid residues, which attract the positive Na⁺ ion and keep out negatively charged ions such as chloride. The cations flow into a more constricted part of the pore that is 0.3 by 0.5 nm wide, which is just large enough to allow a single Na⁺ ion with a water molecule associated to pass through. The larger K⁺ ion cannot fit through this area. Differently sized ions also cannot interact as well with the negatively charged glutamic acid residues that line the pore.

Diversity

Voltage-gated sodium channels normally consist of an alpha subunit that forms the ion conduction pore and one to two beta subunits that have several functions including modulation of channel gating.^[4] Expression of the alpha subunit alone is sufficient to produce a functional channel.

Alpha subunits

Figure 1. Likely evolutionary relationship of the nine known human sodium channels.

The family of sodium channels has nine known members, with amino acid identity >50% in the transmembrane and extracellular loop regions. A standardized nomenclature for sodium channels is currently used and is maintained by the IUPHAR.^[5][6]

The proteins of these channels are named Na_v1.1 through Na_v1.9. The gene names are referred to as SCN1A through SCN11A (the SCN6/7A gene is part of the Na_x sub-family and has uncertain function). The likely evolutionary relationship between these channels, based on the similarity of their amino acid sequences, is shown in figure 1. The individual sodium channels are distinguished not only by differences in their sequence but also by their kinetics and expression profiles. Some of this data is summarized in table 1, below.

Table 1. Nomenclature and some functions of voltage-gated sodium channel alpha subunits

Protein name	Gene	Expression profile	Associated human channelopathies
Nav1.1	SCN1A	Central neurons, [peripheral neurons] and cardiac myocytes	febrile epilepsy, GEFS+, Dravet syndrome (also known as severe myclonic epilepsy of infancy or SMEI), borderline SMEI (SMEB), West syndrome (also known as infantile spasms), Doose syndrome (also known as myoclonic astatic epilepsy), intractable childhood epilepsy with generalized tonic-clonic seizures (ICEGTC), Panayiotopoulos syndrome, familial hemiplegic migraine (FHM), familial autism, Rasmussens's encephalitis and Lennox-Gastaut syndrome[7]
Nav1.2	SCN2A	Central neurons, peripheral neurons	inherited febrile seizures and epilepsy
Nav1.3	SCN3A	Central neurons, peripheral neurons and cardiac myocytes	none known
Nav1.4	SCN4A	Skeletal muscle	hyperkalemic periodic paralysis, paramyotonia congenita, and potassium-aggravated myotonia
Nav1.5	SCN5A	Cardiac myocytes, uninnervated skeletal muscle, central neurons	Long QT syndrome, Brugada syndrome, and idiopathic ventricular fibrillation
Nav1.6	SCN8A	Central neurons, dorsal root ganglia, peripheral neurons, heart, glia cells	none known
Nav1.7	SCN9A	Dorsal root ganglia, sympathetic neurons, Schwann cells, and neuroendocrine cells	erythromelalgia, PEPD and channelopathy-associated insensitivity to pain
Nav1.8	SCN10A	Dorsal root ganglia	none known
Nav1.9	SCN11A	Dorsal root ganglia	none known
Nax	SCN7A	heart, uterus, skeletal muscle, astrocytes, dorsal root ganglion cells	none known

Beta subunits

Sodium channel beta subunits are type 1 transmembrane glycoproteins with an extracellular N-terminus and a cytoplasmic C-terminus. As a member of the Ig superfamily, beta subunits contain a prototypic V-set Ig loop in their extracellular domain. Interestingly, beta subunits share no homology with their counterparts of calcium and potassium channels.^[8] Instead, they are homologous to neural cell adhesion molecules (CAMs) and the large family of L1 CAMs. There are four distinct betas named in order of discovery: SCN1B, SCN2B, SCN3B, SCN4B (table 2). Beta 1 and beta 3 interact with the alpha subunit non-covalently while beta 2 and beta 4 associate with alpha via disulfide bond.^[9]

Role of beta subunits as cell adhesion molecules

In addition to regulating channel gating, sodium channel beta subunits also modulate channel expression and form links to the intracelluar cytoskeleton via ankyrin and spectrin.^[4][10][11] Voltage-gated sodium channels also assemble with a variety of other proteins, such as FHF proteins (Fibroblast growth factor Homologous Factor), calmodulin, cytoskeleton or regulatory kinases^{[12][13][14][15][16]}, which form a complex with sodium channels, influencing its expression and/or function. Several beta subunits interact with one or more extracellular matrix (ECM) molecules. Contactin, also known as F3 or F11, associates with beta 1 as shown via co-immunoprecipitation^[17]. Fibronectin-like (FN-like) repeats of Tenascin-C and Tenascin-R bind with beta 2 in contrast to the Epidermal growth factor-like (EGF-like) repeats that repel beta2.^[18] A disintegrin and metalloproteinase (ADAM) 10 sheds beta 2's ectodomain possibly inducing neurite outgrowth.^[19] Beta 3 and beta 1 bind to neurofascin at Nodes of Ranvier in developing neurons.^[20]

Table 2. Nomenclature and some functions of voltage-gated sodium channel beta subunits

Protein name	Gene link	Assembles with	Expression profile	Associated human channelopathies
Navβ1	SCN1B	Nav1.1 to Nav1.7	Central Neurons, Peripheral Neurons, skeletal muscle, heart, glia	epilepsy (GEFS+)
Navβ2	SCN2B	Nav1.1, Nav1.2, Nav1.5 to Nav1.7	Central Neurons, peripheral neurons, heart, glia	none known
Navβ3	SCN3B	Nav1.1 to Nav1.3, Nav1.5	central neurons, adrenal gland, kidney, peripheral neurons	none known
Navβ4	SCN4B	Nav1.1, Nav1.2, Nav1.5	heart, skeletal muscle, central and peripheral neurons	none known

Ligand-gated

Ligand-gated sodium channels are activated by binding of a ligand instead of a change in membrane potential.

They are found e.g. in the neuromuscular junction as nicotinic receptors, where the ligands are acetylcholine molecules. Most channels of this type are permeable to potassium to some degree as well as to sodium.

Role in action potential

See main article: Action potential

Voltage-gated sodium channels play an important role in action potentials. If enough channels open when there is a change in the cell's membrane potential, a small but significant number of Na⁺ ions will move into the cell down their electrochemical gradient, further depolarizing the cell. Thus, the more Na⁺ channels localized in a region of a cell's membrane, the faster the action potential will propagate, and the more excitable that area of the cell will be. This is an example of a positive feedback loop. The ability of these channels to assume a closed-inactivated state causes the refractory period and is critical for the propagation of action potentials down an axon.

Na⁺ channels both open and close more quickly than K⁺ channels, producing an influx of positive charge (Na⁺) toward the beginning of the action potential and an efflux (K⁺) toward the end.

Ligand-gated sodium channels, on the other hand, create the change in the membrane potential in the first place, in response to the binding of a ligand to it.

Pharmacologic modulation

Blockers

See Sodium channel blockers

Activators

The following naturally produced substances persistently activate (open) sodium channels:

• Alkaloid based toxins
  • aconitine
  • batrachotoxin
  • brevetoxin
  • ciguatoxin
  • delphinine
  • grayanotoxin
  • veratridine

Gating modifiers

The following toxins modify the gating of sodium channels:

• Peptide based toxins
  • μ-conotoxin
  • δ-atracotoxin^[21]
  • Scorpion venom toxins,^[22] such as Birtoxin

See also

Template:Multicol

• Ion channels
• Calcium channels
• Potassium channels

Template:Multicol-break

• Resting ion channels
• Epithelial sodium channel

Template:Multicol-end

References

1. Jessell TM, Kandel ER, Schwartz JH (2000). Principles of Neural Science (4^th ed.). New York: McGraw-Hill. pp. 154–69. ISBN 0-8385-7701-6.
2. Bertil Hillel (2001). Ion Channels of Excitable Membranes (3^rd ed.). Sunderland, Mass: Sinauer. pp. 73–7. ISBN 0-87893-321-2.
3. Yu FH, Catterall WA (2003). "Overview of the voltage-gated sodium channel family". Genome Biol. 4 (3): 207. doi:10.1186/gb-2003-4-3-207. PMC 153452. PMID 12620097.
4. Isom LL (2001). "Sodium channel beta subunits: anything but auxiliary". Neuroscientist. 7 (1): 42–54. doi:10.1177/107385840100700108. PMID 11486343. Cite error: The named reference "Isom" was defined multiple times with different content (see the help page).
5. IUPHAR - International Union of Basic and Clinical Pharmacology
6. Catterall WA, Goldin AL, Waxman SG (2005). "International Union of Pharmacology. XLVII. Nomenclature and structure-function relationships of voltage-gated sodium channels". Pharmacol Rev. 57 (4): 397–409. doi:10.1124/pr.57.4.4. PMID 16382098.
7. Lossin C. "SCN1A infobase". Retrieved 2009-10-30. compilation of genetic variations in the SCN1A gene that alter the expression or function of Nav1.1 {{cite web}}: Cite has empty unknown parameter: |coauthors= (help)
8. Catterall WA (2000). "From ionic currents to molecular mechanisms: the structure and function of voltage-gated sodium channels". Neuron. 26 (1): 13–25. doi:10.1016/S0896-6273(00)81133-2. PMID 10798388. {{cite journal}}: Unknown parameter |month= ignored (help)
9. Isom LL, De Jongh KS, Patton DE, Reber BF, Offord J, Charbonneau H, Walsh K, Goldin AL, Catterall WA (1992). "Primary structure and functional expression of the beta 1 subunit of the rat brain sodium channel". Science. 256 (5058): 839–42. doi:10.1126/science.1375395. PMID 1375395. {{cite journal}}: Unknown parameter |month= ignored (help)
10. Malhotra JD, Kazen-Gillespie K, Hortsch M, Isom LL (2000). "Sodium channel beta subunits mediate homophilic cell adhesion and recruit ankyrin to points of cell-cell contact". J. Biol. Chem. 275 (15): 11383–8. doi:10.1074/jbc.275.15.11383. PMID 10753953. {{cite journal}}: Unknown parameter |month= ignored (help)
11. Malhotra JD, Koopmann MC, Kazen-Gillespie KA, Fettman N, Hortsch M, Isom LL (2002). "Structural requirements for interaction of sodium channel beta 1 subunits with ankyrin". J. Biol. Chem. 277 (29): 26681–8. doi:10.1074/jbc.M202354200. PMID 11997395. {{cite journal}}: Unknown parameter |month= ignored (help)
12. Cantrell AR, Catterall WA (2001). "Neuromodulation of Na+ channels: an unexpected form of cellular plasticity". Nat. Rev. Neurosci. 2 (6): 397–407. doi:10.1038/35077553. PMID 11389473. {{cite journal}}: |access-date= requires |url= (help); Unknown parameter |month= ignored (help)
13. Isom LL (2001). "Sodium channel beta subunits: anything but auxiliary". Neuroscientist. 7 (1): 42–54. doi:10.1177/107385840100700108. PMID 11486343. {{cite journal}}: |access-date= requires |url= (help); Unknown parameter |month= ignored (help)
14. Shah BS, Rush AM, Liu S, Tyrrell L, Black JA, Dib-Hajj SD, Waxman SG (2004). "Contactin associates with sodium channel Nav1.3 in native tissues and increases channel density at the cell surface". J. Neurosci. 24 (33): 7387–99. doi:10.1523/JNEUROSCI.0322-04.2004. PMID 15317864. {{cite journal}}: Unknown parameter |month= ignored (help)
15. Wittmack EK, Rush AM, Craner MJ, Goldfarb M, Waxman SG, Dib-Hajj SD (2004). "Fibroblast growth factor homologous factor 2B: association with Nav1.6 and selective colocalization at nodes of Ranvier of dorsal root axons". J. Neurosci. 24 (30): 6765–75. doi:10.1523/JNEUROSCI.1628-04.2004. PMID 15282281. {{cite journal}}: Unknown parameter |month= ignored (help)
16. Rush AM, Wittmack EK, Tyrrell L, Black JA, Dib-Hajj SD, Waxman SG (2006). "Differential modulation of sodium channel Na(v)1.6 by two members of the fibroblast growth factor homologous factor 2 subfamily". Eur. J. Neurosci. 23 (10): 2551–62. doi:10.1111/j.1460-9568.2006.04789.x. PMID 16817858. {{cite journal}}: Unknown parameter |month= ignored (help)
17. Kazarinova-Noyes, K., et al., Contactin associates with Na+ channels and increases their functional expression. J Neurosci, 2001. 21(19): p. 7517-25
18. Srinivasan J, Schachner M, Catterall WA (1998). "Interaction of voltage-gated sodium channels with the extracellular matrix molecules tenascin-C and tenascin-R". Proc. Natl. Acad. Sci. U.S.A. 95 (26): 15753–7. doi:10.1073/pnas.95.26.15753. PMC 28116. PMID 9861042. {{cite journal}}: Unknown parameter |month= ignored (help)
19. Kim DY, Ingano LA, Carey BW, Pettingell WH, Kovacs DM (2005). "Presenilin/gamma-secretase-mediated cleavage of the voltage-gated sodium channel beta2-subunit regulates cell adhesion and migration". J. Biol. Chem. 280 (24): 23251–61. doi:10.1074/jbc.M412938200. PMID 15833746. {{cite journal}}: Unknown parameter |month= ignored (help)
20. Ratcliffe CF, Westenbroek RE, Curtis R, Catterall WA (2001). "Sodium channel beta1 and beta3 subunits associate with neurofascin through their extracellular immunoglobulin-like domain". J. Cell Biol. 154 (2): 427–34. doi:10.1083/jcb.200102086. PMC 2150779. PMID 11470829. {{cite journal}}: Unknown parameter |month= ignored (help)
21. Grolleau F, Stankiewicz M, Birinyi-Strachan L, Wang XH, Nicholson GM, Pelhate M, Lapied B (2001). "Electrophysiological analysis of the neurotoxic action of a funnel-web spider toxin, delta-atracotoxin-HV1a, on insect voltage-gated Na+ channels". J. Exp. Biol. 204 (Pt 4): 711–21. PMID 11171353.
22. Possani, L.D.; Becerrill, B.; Delepierre, M.; Tytgat Hammock, J. (1999). "Scorpion toxins specific for Na+-channels". European Journal of Biochemistry. 264: 287–300. doi:10.1046/j.1432-1327.1999.00625.x. PMID 10491073.

External links

• Sodium+Channels at the U.S. National Library of Medicine Medical Subject Headings (MeSH)
• "Voltage-Gated Sodium Channels". IUPHAR Database of Receptors and Ion Channels. International Union of Basic and Clinical Pharmacology. {{cite web}}: Cite has empty unknown parameter: |coauthors= (help)