Publication | Open Access
The role of Ca<sup>2+</sup>‐activated K<sup>+</sup> channel spliced variants in the tonotopic organization of the turtle cochlea
104
Citations
35
References
1999
Year
NeurotransmissionCellular PhysiologyHyperpolarization (Biology)Auditory ScienceSplice SitesCa2+ SensitivityCell PhysiologyHealth SciencesAnimal PhysiologyMolecular PhysiologyCochlear NucleiCochlear AnatomyIon ChannelsMorphogenesisAuditory ResearchNervous SystemAuditory Hair CellsBiologyDevelopmental BiologySignal TransductionMultiple IsoformsNeurophysiologyPhysiologyTonotopic OrganizationAuditory PhysiologyCochlear PhysiologyElectrophysiologyCochlear DevelopmentMedicineAuditory SystemTurtle Cochlea
1. Turtle auditory hair cells contain multiple isoforms of the pore-forming alpha-subunit of the large-conductance Ca2+-activated K+ (KCa) channel due to alternative splicing at two sites. Six splice variants were studied by expression in Xenopus oocytes. 2. The isoforms possessed differences in apparent Ca2+ sensitivity and kinetics. The lowest Ca2+ sensitivity was observed in a novel variant resulting from a 26 amino acid deletion around one of the splice sites. 3. Co-expression of a bovine beta-subunit slowed the current relaxation 10-fold compared with channels formed from alpha-subunits alone but preserved the original order of kinetic differences. The beta-subunit also increased the Ca2+ sensitivity of isoforms to bring them nearer the range of sensitivity of the native KCa channels of the hair cell. 4. With channels formed from alpha-subunits or alpha + beta-subunits, the half-activation voltage in a fixed Ca2+ concentration, and the time constant of the current relaxation, varied linearly with the combined size of the insertions/deletions at the splice sites. 5. Experiments in which the beta/alpha concentration ratio was varied indicated that the beta-subunit exerts an all-or-none effect on the Ca2+ sensitivity and kinetics of the channel. 6. Co-expression of an avian beta2-subunit had effects on kinetics and Ca2+ sensitivity of several alpha-isoforms which were qualitatively similar to those produced by the bovine beta-subunit. 7. We conclude that differential expression of alternatively spliced alpha-subunit variants and a non-uniform distribution of a beta-subunit can produce a range of KCa channel properties needed to explain the tonotopic organization of the turtle cochlea.
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