Pharmacology of A-Type K+ Channels
- PMID: 33907894
- DOI: 10.1007/164_2021_456
Pharmacology of A-Type K+ Channels
Abstract
Transient outward potassium currents were first described nearly 60 years ago, since then major strides have been made in understanding their molecular basis and physiological roles. From the large family of voltage-gated potassium channels members of 3 subfamilies can produce such fast-inactivating A-type potassium currents. Each subfamily gives rise to currents with distinct biophysical properties and pharmacological profiles and a simple workflow is provided to aid the identification of channels mediating A-type currents in native cells. Their unique properties and regulation enable A-type K+ channels to perform varied roles in excitable cells including repolarisation of the cardiac action potential, controlling spike and synaptic timing, regulating dendritic integration and long-term potentiation as well as being a locus of neural plasticity.
Keywords: A-type K+ channel; Kv1.4; Kv3.4; Kv4; Potassium channel; Voltage-clamp.
© 2021. The Author(s), under exclusive license to Springer Nature Switzerland AG.
References
-
- Amadi CC, Brust RD, Skerritt MR, Campbell DL (2007) Regulation of Kv4.3 closed state inactivation and recovery by extracellular potassium and intracellular KChIP2b. Channels (Austin) 1:305–314
-
- Anderson D, Mehaffey WH, Iftinca M, Rehak R, Engbers JD, Hameed S, Zamponi GW, Turner RW (2010a) Regulation of neuronal activity by Cav3-Kv4 channel signaling complexes. Nat Neurosci 13:333–337 - PubMed
-
- Anderson D, Rehak R, Hameed S, Mehaffey WH, Zamponi GW, Turner RW (2010b) Regulation of the KV4.2 complex by CaV3.1 calcium channels. Channels (Austin) 4:163–167
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