Kv3.3 Channels at the Purkinje Cell Soma Are Necessary for Generation of the Classical Complex Spike Waveform

doi:10.1523/JNEUROSCI.4358-07.2008

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The Journal of Neuroscience, February 6, 2008, 28(6):1291-1300; doi:10.1523/JNEUROSCI.4358-07.2008

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Cellular/Molecular
Kv3.3 Channels at the Purkinje Cell Soma Are Necessary for Generation of the Classical Complex Spike Waveform
Edward Zagha,¹^,3^,4 Eric J. Lang,¹ and Bernardo Rudy¹^,2^,3
Departments of ¹Physiology and Neuroscience and ²Biochemistry, ³Smilow Neuroscience Program, and ⁴Medical Scientist Training Program, New York University School of Medicine, New York, New York 10016
Correspondence should be addressed to Dr. Bernardo Rudy, Smilow Neuroscience Program, New York University School of Medicine, 522 First Avenue, Sixth Floor, New York, NY 10016. Email: rudyb01{at}med.nyu.edu
Voltage-gated potassium channel subunit Kv3.3 is prominentlyexpressed in cerebellar Purkinje cells and is known to be importantfor cerebellar function, as human and mouse movement disordersresult from mutations in Kv3.3. To understand these behavioraldeficits, it is necessary to know the role of Kv3.3 channelson the physiological responses of Purkinje cells. We studiedthe function of Kv3.3 channels in regulating the synapticallyevoked Purkinje cell complex spike, the massive postsynapticresponse to the activation of climbing fiber afferents, believedto be fundamental to cerebellar physiology. Acute slice recordingsrevealed that Kv3.3 channels are required for generation ofthe repetitive spikelets of the complex spike. We found thatspikelet expression is regulated by somatic, and not by dendritic,Kv3 activity, which is consistent with dual somatic–dendriticrecordings that demonstrate spikelet generation at axosomaticmembranes. Simulations of Purkinje cell Na⁺ currents show thatthe unique electrical properties of Kv3 and resurgent Na⁺ channelsare coordinated to limit accumulation of Na⁺ channel inactivationand enable rapid, repetitive firing. We additionally show thatKv3.3 knock-out mice produce altered complex spikes in vitroand in vivo, which is likely a cellular substrate of the cerebellarphenotypes observed in these mice. This characterization presentsnew tools to study complex spike function, cerebellar signaling,and Kv3.3-dependent human and mouse phenotypes.

Key words: Kv3; potassium channels; Purkinje cell; complex spike; spinocerebellar ataxia; excitability

Received Sept. 23, 2007; revised Dec. 17, 2007; accepted Dec. 18, 2007.

Correspondence should be addressed to Dr. Bernardo Rudy, Smilow Neuroscience Program, New York University School of Medicine, 522 First Avenue, Sixth Floor, New York, NY 10016. Email: rudyb01{at}med.nyu.edu

This article has been cited by other articles:

J. T. Davie, B. A. Clark, and M. Hausser
The Origin of the Complex Spike in Cerebellar Purkinje Cells
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