Inhibition of Navβ4 Peptide-Mediated Resurgent Sodium Currents in Nav1.7 Channels by Carbamazepine, Riluzole, and Anandamide

Theile, Jonathan W.; Cummins, Theodore R.

doi:10.1124/mol.111.072751

Cited by 67 publications

(69 citation statements)

References 38 publications

(68 reference statements)

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“…1D, n 5 4), tested with a protocol using 30-millisecond test pulses to 220 mV delivered every 3 seconds from a holding potential of 275 mV. As expected, carbamazepine block was strongly use dependent (Willow et al, 1985;Theile and Cummins, 2011), with block greatly enhanced by stimulating at 10, rather than 0.33 Hz, and was also strongly voltage dependent (Kuo et al, 1997;Kuo, 1998), with the steadystate inactivation curve shifted approximately 20 mV in the hyperpolarizing direction by 100 mM carbamazepine (data not shown).…”

Section: Resultsmentioning

confidence: 99%

Sidedness of Carbamazepine Accessibility to Voltage-Gated Sodium Channels

Bean

2013

Mol Pharmacol

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Voltage-gated sodium channels are inhibited by many local anesthetics, antiarrhythmics, and antiepileptic drugs. The local anesthetic lidocaine appears to be able to access its binding site in the sodium channel only from the membrane phase or from the internal face of the channel. In contrast, the antiepileptic drug carbamazepine was found to inhibit voltage-gated sodium channels only with external, but not internal, application, implying a major difference. We investigated this point using both wholecell and inside-out patch recordings from human Na v 1.7 channels in a stable cell line. In the whole-cell configuration, carbamazepine inhibited sodium current within seconds when applied externally, but had little or no effect when applied internally for up to 15 minutes, confirming previous results. However, carbamazepine inhibited sodium channels effectively and rapidly when applied to the internal face of the membrane using inside-out patch recording. We found that lidocaine also has little or no effect when applied intracellularly in whole-cell recording, but blocks effectively and rapidly when applied to the internal surface using inside-out patches. In contrast, the cationic lidocaine derivative QX-314 (N-ethyl-lidocaine) blocks effectively when applied internally with whole-cell dialysis, as well as when applied to insideout patches. We conclude that carbamazepine and lidocaine access the sodium channel in similar ways and hypothesize that their lack of effect with internal dialysis in whole-cell recording reflects rapid exit through membrane near the pipette recording site. This effect likely limits the ability of any compound with significant membrane permeability to be applied intracellularly by whole-cell dialysis.

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Section: Resultsmentioning

confidence: 99%

Sidedness of Carbamazepine Accessibility to Voltage-Gated Sodium Channels

Bean

2013

Mol Pharmacol

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“…Subsequent knockdown of β4 expression using siRNA in CGNs resulted in reduced resurgent sodium current and decreased repetitive firing, providing further evidence for β4 as the open-channel blocking particle (Bant and Raman 2010). A peptide corresponding to β4 was sufficient to invoke resurgent sodium current in HEK 293 cells (Theile and Cummins 2011), again strongly suggesting a role for β4 in the generation of resurgent sodium current in vivo. Importantly, however, co-expression of full-length β4 and Nav1.6 subunits was not sufficient to generate resurgent current , suggesting that key cellular processes, possibly including posttranslational modification, that allow β4 subunits to participate as the open-channel blocking particle may be specific to neurons.…”

Section: Role Of Vgsc B Subunits In Resurgent Sodium Currentmentioning

confidence: 94%

The Role of Non-pore-Forming β Subunits in Physiology and Pathophysiology of Voltage-Gated Sodium Channels

Isom

2014

Voltage Gated Sodium Channels

107

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Voltage-gated sodium channel β1 and β2 subunits were discovered as auxiliary proteins that co-purify with pore-forming α subunits in brain. The other family members, β1B, β3, and β4, were identified by homology and shown to modulate sodium current in heterologous systems. Work over the past 2 decades, however, has provided strong evidence that these proteins are not simply ancillary ion channel subunits, but are multifunctional signaling proteins in their own right, playing both conducting (channel modulatory) and nonconducting roles in cell signaling. Here, we discuss evidence that sodium channel β subunits not only regulate sodium channel function and localization but also modulate voltage-gated potassium channels. In their nonconducting roles, VGSC β subunits function as immunoglobulin superfamily cell adhesion molecules that modulate brain development by influencing cell proliferation and migration, axon outgrowth, axonal fasciculation, and neuronal pathfinding. Mutations in genes encoding β subunits are linked to paroxysmal diseases including epilepsy, cardiac arrhythmia, and sudden infant death syndrome. Finally, β subunits may be targets for the future development of novel therapeutics.

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“…7 Cell Line in a Ubc9-dependent Manner-Because we could not pharmacologically or genetically isolate NaV1.1 and NaV1.3 currents, which account for Ͻ15% of the CAD cell sodium current, we chose to test the importance of CRMP2-SUMOylation in NaV1.7 trafficking in a HEK293 cell line expressing only NaV1.7 channels (38). Representative traces of NaV1.7 currents from these cells are illustrated in Fig.…”

Section: Journal Of Biological Chemistry 24321mentioning

confidence: 99%

CRMP2 Protein SUMOylation Modulates NaV1.7 Channel Trafficking

Dustrude

Wilson

et al. 2013

Journal of Biological Chemistry

126

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Background: Post-translational modifications of CRMP2 protein direct its regulation of effector proteins. Results: Destruction of a CRMP2 SUMOylation site reduces surface expression and current density of sodium channel NaV1.7. Conclusion: CRMP2 SUMOylation choreographs NaV1.7, but not NaV1.1 or NaV1.3, trafficking. Significance: Learning how neuronal NaV1.7 trafficking is modulated by CRMP2 is important for understanding the mechanism of action of NaV-targeted anti-epileptic and anti-nociceptive drugs.

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Inhibition of Navβ4 Peptide-Mediated Resurgent Sodium Currents in Nav1.7 Channels by Carbamazepine, Riluzole, and Anandamide

Cited by 67 publications

References 38 publications

Sidedness of Carbamazepine Accessibility to Voltage-Gated Sodium Channels

Sidedness of Carbamazepine Accessibility to Voltage-Gated Sodium Channels

The Role of Non-pore-Forming β Subunits in Physiology and Pathophysiology of Voltage-Gated Sodium Channels

CRMP2 Protein SUMOylation Modulates NaV1.7 Channel Trafficking

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