PR01497

SHALCHANNEL

PRINTS entry
Member databasePRINTS
PRINTS typefamily
Short nameSHALCHANNEL

Description
Imported from IPR003975

The Kv family can be divided into several subfamilies on the basis of sequence similarity and function. Four of these subfamilies, Kv1 (Shaker), Kv2 (Shab), Kv3 (Shaw) and Kv4 (Shal), consist of pore-forming alpha subunits that associate with different types of beta subunit. Each alpha subunit comprises six hydrophobic TM domains with a P-domain between the fifth and sixth, which partially resides in the membrane. The fourth TM domain has positively charged residues at every third residue and acts as a voltage sensor, which triggers the conformational change that opens the channel pore in response to a displacement in membrane potential
[9]
. More recently, 4 new electrically-silent alpha subunits have been cloned: Kv5 (KCNF), Kv6 (KCNG), Kv8 and Kv9 (KCNS). These subunits do not themselves possess any functional activity, but appear to form heteromeric channels with Kv2 subunits, and thus modulate Shab channel activity
[2]
. When highly expressed, they inhibit channel activity, but at lower levels show more specific modulatory actions.

The Shal potassium channel was found in Drosophila melanogaster (Fruit fly). Several vertebrate potassium channels with similar amino acid sequences were subsequently found and, together with the D. melanogaster Shal channel, now constitute the Kv4 family. These channels are the primary subunits contributing to transient, voltage-dependent potassium currents in the nervous system (A currents) and the heart (transient outward current), and are inhibited by free fatty acids
[1]
. This family can be further divided into 3 subfamilies, designated Kv4.1(KCND1), Kv4.2(KCND2) and Kv4.3(KCND3).

Potassium channels are the most diverse group of the ion channel family
[10, 4]
. They are important in shaping the action potential, and in neuronal excitability and plasticity
[7]
. The potassium channel family is composed of several functionally distinct isoforms, which can be broadly separated into 2 groups
[5]
: the practically non-inactivating 'delayed' group and the rapidly inactivating 'transient' group.

These are all highly similar proteins, with only small amino acid changes causing the diversity of the voltage-dependent gating mechanism, channel conductance and toxin binding properties. Each type of K+channel is activated by different signals and conditions depending on their type of regulation: some open in response to depolarisation of the plasma membrane; others in response to hyperpolarisation or an increase in intracellular calcium concentration; some can be regulated by binding of a transmitter, together with intracellular kinases; while others are regulated by GTP-binding proteins or other second messengers
[8]
. In eukaryotic cells, K+channels are involved in neural signalling and generation of the cardiac rhythm, act as effectors in signal transduction pathways involving G protein-coupled receptors (GPCRs) and may have a role in target cell lysis by cytotoxic T-lymphocytes
[6]
. In prokaryotic cells, they play a role in the maintenance of ionic homeostasis
[3]
.

All K+channels discovered so far possess a core of alpha subunits, each comprising either one or two copies of a highly conserved pore loop domain (P-domain). The P-domain contains the sequence (T/SxxTxGxG), which has been termed the K+selectivity sequence. In families that contain one P-domain, four subunits assemble to form a selective pathway for K+across the membrane. However, it remains unclear how the 2 P-domain subunits assemble to form a selective pore. The functional diversity of these families can arise through homo-or hetero-associations of alpha subunits or association with auxiliary cytoplasmic beta subunits. K+channel subunits containing one pore domain can be assigned into one of two superfamilies: those that possess six transmembrane (TM) domains and those that possess only two TM domains. The six TM domain superfamily can be further subdivided into conserved gene families: the voltage-gated (Kv) channels; the KCNQ channels (originally known as KvLQT channels); the EAG-like K+channels; and three types of calcium (Ca)-activated K+channels (BK, IK and SK)
[3]
. The 2TM domain family comprises inward-rectifying K+channels. In addition, there are K+channel alpha-subunits that possess two P-domains. These are usually highly regulated K+selective leak channels.

References
Imported from IPR003975

1.Structure and function of Kv4-family transient potassium channels. Birnbaum SG, Varga AW, Yuan LL, Anderson AE, Sweatt JD, Schrader LA. Physiol. Rev. 84, 803-33, (2004). View articlePMID: 15269337

2.New modulatory alpha subunits for mammalian Shab K+ channels. Salinas M, Duprat F, Heurteaux C, Hugnot JP, Lazdunski M. J. Biol. Chem. 272, 24371-9, (1997). View articlePMID: 9305895

3.An overview of the potassium channel family. Miller C. Genome Biol. 1, REVIEWS0004, (2000). View articlePMID: 11178249

4.Shaw-like rat brain potassium channel cDNA's with divergent 3' ends. Luneau C, Wiedmann R, Smith JS, Williams JB. FEBS Lett. 288, 163-7, (1991). View articlePMID: 1879548

5.Molecular basis of functional diversity of voltage-gated potassium channels in mammalian brain. Stuhmer W, Ruppersberg JP, Schroter KH, Sakmann B, Stocker M, Giese KP, Perschke A, Baumann A, Pongs O. EMBO J. 8, 3235-44, (1989). View articlePMID: 2555158

6.Cloning, functional expression, and regulation of two K+ channels in human T lymphocytes. Attali B, Romey G, Honore E, Schmid-Alliana A, Mattei MG, Lesage F, Ricard P, Barhanin J, Lazdunski M. J. Biol. Chem. 267, 8650-7, (1992). View articlePMID: 1373731

7.Cloning of a probable potassium channel gene from mouse brain. Tempel BL, Jan YN, Jan LY. Nature 332, 837-9, (1988). View articlePMID: 2451788

8.Multiple potassium-channel components are produced by alternative splicing at the Shaker locus in Drosophila. Schwarz TL, Tempel BL, Papazian DM, Jan YN, Jan LY. Nature 331, 137-42, (1988). View articlePMID: 2448635

9.Potassium channels: watching a voltage-sensor tilt and twist. Sansom MS. Curr. Biol. 10, R206-9, (2000). View articlePMID: 10712896

10.The molecular biology of K+ channels. Perney TM, Kaczmarek LK. Curr. Opin. Cell Biol. 3, 663-70, (1991). View articlePMID: 1772658

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