2013
DOI: 10.1113/jphysiol.2013.251983
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Kv3 channel assembly, trafficking and activity are regulated by zinc through different binding sites

Abstract: Key points• Kv3 channels play a critical role in neuronal fast spiking and their regulation can profoundly influence the functions of various neural circuits.• Zinc reversibly inhibits fast spiking in cultured neurons by inhibiting Kv3 channels. Surprisingly, we found that the zinc inhibition is not through its known site in the N-terminal T1 domain of Kv3.1.• We have identified a new zinc-binding site in the Kv3.1 C-terminus, involved in regulating channel activity and targeting, but not the zinc inhibition.•… Show more

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Cited by 15 publications
(21 citation statements)
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“…In addition to altering axonal targeting, this mutation also slowed the time constant of activation of Kv3.1b channels and altered voltage dependence. In contrast, mutation of the other two histidine residues downstream of the targeting motif did not affect trafficking into the axon, or significantly impact voltage dependence or kinetics (87). Thus the function of these two downstream sites is not yet known.…”
Section: Modulation Of Kv31 Channels By Zincmentioning
confidence: 86%
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“…In addition to altering axonal targeting, this mutation also slowed the time constant of activation of Kv3.1b channels and altered voltage dependence. In contrast, mutation of the other two histidine residues downstream of the targeting motif did not affect trafficking into the axon, or significantly impact voltage dependence or kinetics (87). Thus the function of these two downstream sites is not yet known.…”
Section: Modulation Of Kv31 Channels By Zincmentioning
confidence: 86%
“…Histidine residues at these sites are essential for metal binding, and simultaneous mutation of all three histidines fully abolishes zinc binding (87). In the Kv3.1b channel isoform, mutation of the histidine located within the axonal targeting motif abolished targeting of Kv3.1b to the axon, suggesting that zinc binding at this site controls either the interaction of the targeting motif with ankyrin G or with the NH 2 terminus of the Kv3.1 channel (87). In addition to altering axonal targeting, this mutation also slowed the time constant of activation of Kv3.1b channels and altered voltage dependence.…”
Section: Modulation Of Kv31 Channels By Zincmentioning
confidence: 99%
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“…Whole-cell patch-clamp recording was performed on BMDM obtained from WT and Trpm2 −/− mice, using the same internal solution, Hank’s buffer, recording protocols and the setup as previously described 57 . In voltage-clamp recording, the cells were initially held at −80 mV, given 200-ms voltage episodes in 10-mV increment from −100 mV to +100 mV, and then the I-V relationship was obtained.…”
Section: Methodsmentioning
confidence: 99%
“…Increase in A‐type potassium current due to hypothyroidism was accompanied by decreased AP width, lower repolarization potential and increased number of APs in a series (Sanchez‐Alonso et al ., ). In a primary culture of hippocampal neurons, increased expression of K V 3.1 channels increased the firing activity (Martina et al ., ; Gu et al ., ) and inhibition of those channels attenuated AP firing (Gu et al ., ).…”
Section: Discussionmentioning
confidence: 97%