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Journal ArticleDOI

The Antipsychotic Drug Loxapine Is an Opener of the Sodium-Activated Potassium Channel Slack (Slo2.2)

TLDR
In dorsal root ganglion neurons, loxapine was found to behave as an opener of native KNa channels and to increase the rheobase of action potential.
Abstract
Sodium-activated potassium (K(Na)) channels have been suggested to set the resting potential, to modulate slow after-hyperpolarizations, and to control bursting behavior or spike frequency adaptation (Trends Neurosci 28:422-428, 2005). One of the genes that encodes K(Na) channels is called Slack (Kcnt1, Slo2.2). Studies found that Slack channels were highly expressed in nociceptive dorsal root ganglion neurons and modulated their firing frequency (J Neurosci 30:14165-14172, 2010). Therefore, Slack channel openers are of significant interest as putative analgesic drugs. We screened the library of pharmacologically active compounds with recombinant human Slack channels expressed in Chinese hamster ovary cells, by using rubidium efflux measurements with atomic absorption spectrometry. Riluzole at 500 μM was used as a reference agonist. The antipsychotic drug loxapine and the anthelmintic drug niclosamide were both found to activate Slack channels, which was confirmed by using manual patch-clamp analyses (EC(50) = 4.4 μM and EC(50) = 2.9 μM, respectively). Psychotropic drugs structurally related to loxapine were also evaluated in patch-clamp experiments, but none was found to be as active as loxapine. Loxapine properties were confirmed at the single-channel level with recombinant rat Slack channels. In dorsal root ganglion neurons, loxapine was found to behave as an opener of native K(Na) channels and to increase the rheobase of action potential. This study identifies new K(Na) channel pharmacological tools, which will be useful for further Slack channel investigations.

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Citations
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Journal ArticleDOI

Slack, Slick, and Sodium-Activated Potassium Channels

TL;DR: This review covers the cellular and molecular properties of Slack and Slick channels and compares them with findings on the properties of sodium-activated potassium currents in native neurons, suggesting that KNa channels play a central role in neuronal plasticity and intellectual function.
Journal ArticleDOI

Control of somatic membrane potential in nociceptive neurons and its implications for peripheral nociceptive transmission.

TL;DR: This study deciphers a complement of ion channels that sets the somatic Erest of nociceptive neurons and provides strong evidence for a robust filtering role of the somata of afferent fibres conveying somatosensory inputs to the central nervous system.
Journal ArticleDOI

International Union of Basic and Clinical Pharmacology. C. Nomenclature and Properties of Calcium-Activated and Sodium-Activated Potassium Channels

TL;DR: The molecular relationships between these channels are described and a new nomenclature is introduced that differentiates between calcium- and sodium-activated potassium channels.
Journal ArticleDOI

An Epilepsy-Associated KCNT1 Mutation Enhances Excitability of Human iPSC-Derived Neurons by Increasing Slack KNa Currents.

TL;DR: This study is the first demonstration that a KCNT1 mutation increases the Slack current in neurons, and provides the first explanation for how this increased potassium current induces hyperexcitability, which could be the underlining factor causing seizures.
Journal ArticleDOI

Slack Channels Expressed in Sensory Neurons Control Neuropathic Pain in Mice

TL;DR: Global and sensory neuron-specific Slack mutant mice generated and analyzed their behavior in various animal models of pain suggest that modulating its activity might represent a novel strategy for management of neuropathic pain.
References
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Journal ArticleDOI

Crystal structure and mechanism of a calcium-gated potassium channel

TL;DR: This work has cloned, expressed, analysed electrical properties, and determined the crystal structure of a K+ channel (MthK) from Methanobacterium thermoautotrophicum in the Ca2+-bound, opened state.
Journal ArticleDOI

Modelling schizophrenia using human induced pluripotent stem cells.

TL;DR: HiPSC neuronal phenotypes and gene expression changes associated with SCZD, a complex genetic psychiatric disorder, were reported and key cellular and molecular elements of theSCZD phenotype were ameliorated following treatment of SCZC hiPSC neurons with the antipsychotic loxapine.
Journal ArticleDOI

Eight potassium channel families revealed by the C. elegans genome project

TL;DR: Novel families of potassium channel genes were revealed, as well as conserved homologues of all known vertebrate families, and an exceptionally large class of at least 23 genes with a novel subunit structure having two tandem 'P' domains are revealed.
Journal Article

The neuroprotective agent riluzole activates the two P domain K(+) channels TREK-1 and TRAAK.

TL;DR: It is reported that riluzole is an activator of TREK-1 and TRAAK, two important members of a new structural family of mammalian background K(+) channels with four transmembrane domains and two pore regions.
Journal ArticleDOI

The Sodium-Activated Potassium Channel Is Encoded by a Member of the Slo Gene Family

TL;DR: It is demonstrated in C. elegans that slo-2 mutants are hypersensitive to hypoxia, suggesting a conserved role for the slO-2 gene subfamily.
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