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

Cloxyquin has been reported as a specific activator of TRESK (K2P18.1, TWIK-related spinal cord K+ channel) background potassium channel. In this study, we have synthetized chemically modified analogues of cloxyquin and tested their effects on TRESK and other K2P channels. The currents of murine K2P...

Teljes leírás

Elmentve itt :
Bibliográfiai részletek
Szerzők: Lengyel Miklós
Erdélyi Ferenc
Pergel Enikő
Bálint-Polonka Ágnes
Dobolyi Alice
Bozsaki Péter
Dux Mária
Király Kornél
Hegedűs Tamás
Czirják Gábor
Mátyus Péter
Enyedi Péter
Dokumentumtípus: Cikk
Megjelent: 2019
Sorozat:MOLECULAR PHARMACOLOGY 95 No. 6
doi:10.1124/mol.118.115626

mtmt:30654928
Online Access:http://publicatio.bibl.u-szeged.hu/17627
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245 1 0 |a Chemically Modified Derivatives of the Activator Compound Cloxyquin Exert Inhibitory Effect on TRESK (K2P18.1) Background Potassium Channel  |h [elektronikus dokumentum] /  |c  Lengyel Miklós 
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490 0 |a MOLECULAR PHARMACOLOGY  |v 95 No. 6 
520 3 |a Cloxyquin has been reported as a specific activator of TRESK (K2P18.1, TWIK-related spinal cord K+ channel) background potassium channel. In this study, we have synthetized chemically modified analogues of cloxyquin and tested their effects on TRESK and other K2P channels. The currents of murine K2P channels, expressed heterologously in Xenopus oocytes, were measured by two-electrode voltage clamp, whereas the native background K+ conductance of mouse dorsal root ganglion (DRG) neurons was examined by the whole-cell patch clamp method. Some of the analogues retained the activator character of the parent compound, but more interestingly, other derivatives inhibited mouse TRESK current. The inhibitor analogues (A2764 and A2793) exerted state-dependent effect. The degree of inhibition by 100 µM A2764 (77.8±1.5%, n=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±4.3% inhibition, n=7). The selectivity of the inhibitor compounds was tested on several K2P channels. A2793 inhibited TASK-1 (100 µM, 53.4±6%, n=5), while A2764 was more selective for TRESK, it only moderately influenced TREK-1 and TALK-1. The effect of A2764 was also examined on the background K+ currents of DRG neurons. A subpopulation of DRG neurons, prepared from wild-type animals, expressed background K+ currents sensitive to A2764, while 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. 
700 0 1 |a Erdélyi Ferenc  |e aut 
700 0 1 |a Pergel Enikő  |e aut 
700 0 2 |a Bálint-Polonka Ágnes  |e aut 
700 0 2 |a Dobolyi Alice  |e aut 
700 0 2 |a Bozsaki Péter  |e aut 
700 0 2 |a Dux Mária  |e aut 
700 0 2 |a Király Kornél  |e aut 
700 0 2 |a Hegedűs Tamás  |e aut 
700 0 2 |a Czirják Gábor  |e aut 
700 0 2 |a Mátyus Péter  |e aut 
700 0 2 |a Enyedi Péter  |e aut 
856 4 0 |u http://publicatio.bibl.u-szeged.hu/17627/1/652.full.pdf  |z Dokumentum-elérés  

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