Mixing and matching TREK/TRAAK subunits generate heterodimeric K
            <sub>2P</sub>
            channels with unique properties

Blin, Sandy; Soussia, Ismail Ben; Kim, Eun Jin; Brau, Frédéric; Kang, Dawon; Lesage, Florian; Bichet, Delphine

doi:10.1073/pnas.1522748113

Cited by 63 publications

(77 citation statements)

References 41 publications

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“…We have previously described that RR inhibits background K 1 currents in DRG neurons (Braun et al, 2015). The molecular correlates of the RRsensitive K 1 current may be TREK-2, TASK-3, or TRAAK homodimers, or heterodimers of the TREK subfamily (Braun et al, 2015;Blin et al, 2016;Lengyel et al, 2016). We found that in neurons derived from wild-type animals, A2764 strongly inhibited the background K 1 current in a subset of DRG neurons.…”

Section: Discussionmentioning

confidence: 59%

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K_2P18.1) Background Potassium Channel

et al. 2019

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Cloxyquin has been reported as a specific activator of TRESK [TWIK-related spinal cord K 1 channel (also known as K 2P 18.1)] background potassium channel. In this study, we have synthetized chemically modified analogs of cloxyquin and tested their effects on TRESK and other K 2P channels. The currents of murine K 2P channels, expressed heterologously in Xenopus oocytes, were measured by two-electrode voltage clamp, whereas the native background K 1 conductance of mouse dorsal root ganglion (DRG) neurons was examined by the whole-cell patch-clamp method. Some of the analogs retained the activator character of the parent compound, but, more interestingly, other derivatives inhibited mouse TRESK current. The inhibitor analogs (A2764 and A2793) exerted state-dependent effects. The degree of inhibition by 100 mM A2764 (77.8% 6 3.5%, n 5 6) was larger in the activated state of TRESK (i.e., after calcineurin-dependent stimulation) than in the resting state of the channel (42.8% 6 11.5% inhibition, n 5 7). The selectivity of the inhibitor compounds was tested on several K 2P channels. A2793 inhibited TWIKrelated acid-sensitive K 1 channel (TASK)-1 (100 mM, 53.4% 6 13, 5%, n 5 5), while A2764 was more selective for TRESK, it only moderately influenced TREK-1 and TWIK-related alkaline pH-activated K 1 channel. The effect of A2764 was also examined on the background K 1 currents of DRG neurons. A subpopulation of DRG neurons, prepared from wild-type animals, expressed background K 1 currents sensitive to A2764, whereas the inhibitor did not affect the currents in the DRG neurons of TRESK-deficient mice. Accordingly, A2764 may prove to be useful for the identification of TRESK current in native cells, and for the investigation of the role of the channel in nociception and migraine. SIGNIFICANCE STATEMENTTRESK background potassium channel is a potential pharmacological target in migraine and neuropathic pain. In this study, we have identified a selective inhibitor of TRESK, A2764. This compound can inhibit TRESK in native cells, leading to cell depolarization and increased excitability. This new inhibitor may be of use to probe the role of TRESK channel in migraine and nociception.

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Section: Discussionmentioning

confidence: 59%

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K_2P18.1) Background Potassium Channel

et al. 2019

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“…Note Added in Proof-While this paper was under review, other authors have published results showing heteromerization of channels in the TREK K 2P subfamily (38,39). These studies reached the same conclusion by using different methods.…”

Section: Acknowledgments-the Skillful Technical Assistance Of Irén Vementioning

confidence: 69%

Formation of Functional Heterodimers by TREK-1 and TREK-2 Two-pore Domain Potassium Channel Subunits

Lengyel

Czirják

Enyedi

2016

Journal of Biological Chemistry

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“…Kim (2003) reviewed the main characteristics of the modulation of two-pore domain K + channels by FFA (TREK-1, TREK-2, and TRAAK). These channels, activated by GPCRs, stretch, pH, and PUFA, are broadly expressed in the nervous system where they control neuronal excitability (Lee et al, 2011; Liu et al, 2014; Blin et al, 2016). The effect of PUFA on TREK channels has profound physiological implications, since TREK-1 was shown to mediate the neuroprotection induced by PUFA (Lauritzen et al, 2000; Heurteaux et al, 2004; Noël et al, 2011; Liu et al, 2014).…”

Section: Ffa Effects On Voltage-gated Ion Channelsmentioning

confidence: 99%

Fatty Acid Regulation of Voltage- and Ligand-Gated Ion Channel Function

Antollini

Barrantes

2016

Front. Physiol.

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Free fatty acids (FFA) are essential components of the cell, where they play a key role in lipid and carbohydrate metabolism, and most particularly in cell membranes, where they are central actors in shaping the physicochemical properties of the lipid bilayer and the cellular adaptation to the environment. FFA are continuously being produced and degraded, and a feedback regulatory function has been attributed to their turnover. The massive increase observed under some pathological conditions, especially in brain, has been interpreted as a protective mechanism possibly operative on ion channels, which in some cases is of stimulatory nature and in other cases inhibitory. Here we discuss the correlation between the structure of FFA and their ability to modulate protein function, evaluating the influence of saturation/unsaturation, number of double bonds, and cis vs. trans isomerism. We further focus on the mechanisms of FFA modulation operating on voltage-gated and ligand-gated ion channel function, contrasting the still conflicting evidence on direct vs. indirect mechanisms of action.

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Mixing and matching TREK/TRAAK subunits generate heterodimeric K _2P channels with unique properties

Cited by 63 publications

References 41 publications

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K_2P18.1) Background Potassium Channel

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K_2P18.1) Background Potassium Channel

Formation of Functional Heterodimers by TREK-1 and TREK-2 Two-pore Domain Potassium Channel Subunits

Fatty Acid Regulation of Voltage- and Ligand-Gated Ion Channel Function

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Mixing and matching TREK/TRAAK subunits generate heterodimeric K 2P channels with unique properties

Cited by 63 publications

References 41 publications

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K2P18.1) Background Potassium Channel

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K2P18.1) Background Potassium Channel

Formation of Functional Heterodimers by TREK-1 and TREK-2 Two-pore Domain Potassium Channel Subunits

Fatty Acid Regulation of Voltage- and Ligand-Gated Ion Channel Function

Contact Info

Product

Resources

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Mixing and matching TREK/TRAAK subunits generate heterodimeric K _2P channels with unique properties

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K_2P18.1) Background Potassium Channel

Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K_2P18.1) Background Potassium Channel