KCNC1

K_v3.1 and K_v3.2 channels are prominently expressed in neurons that fire at high frequency. K_v3.1 channels are prominently expressed in brain (cerebellum > globus pallidus, subthalamic nucleus, substantia nigra > reticular thalamic nuclei, cortical and hippocampal interneurons > inferior colliculi, cochlear and vestibular nuclei), and in retinal ganglion cells.^[8][9][10]

K_v3.1/K_v3.2 conductance is necessary and kinetically optimized for high-frequency action potential generation.^[9][11] K_v3.1 channels are important for the high-firing frequency of auditory and fast-spiking GABAergic interneurons, retinal ganglion cells; regulation of action potential duration in presynaptic terminals.^[8][10]

K_v3.1 currents in heterologous systems are highly sensitive to external tetraethylammonium (TEA) or 4-aminopyridine (4-AP) (IC₅₀ values are 0.2 mM and 29 μM respectively).^[9][10] This can be useful in identifying native channels.^[9] The overlapping sensitivity of potassium current to both 0.5 mM TEA and 30 μM 4-AP strongly suggest an action on K_v3.1 subunits.^[12]

There are two transcript variants of K_v3.1 gene: K_v3.1a and K_v3.1b. K_v3.1 isoforms differ only in their C-terminal sequence.^[13]

A missense mutation c.959G>A (p.Arg320His) in KCNC1 causes progressive myoclonus epilepsy.^[14]

• Voltage-gated potassium channel