Retigabine holds K^sub V^7 channels open and stabilizes the resting potential
The anticonvulsant Retigabine is a K...7 channel agonist used to treat hyperexcitability disorders in humans. Retigabine shifts the voltage dependence for activation of the heteromeric K...7.2/K...7.3 channel to more negative potentials, thus facilitating activation. Although the molecular mechanism...
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Veröffentlicht in: | The Journal of general physiology 2016-03, Vol.147 (3), p.229 |
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Sprache: | eng |
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Zusammenfassung: | The anticonvulsant Retigabine is a K...7 channel agonist used to treat hyperexcitability disorders in humans. Retigabine shifts the voltage dependence for activation of the heteromeric K...7.2/K...7.3 channel to more negative potentials, thus facilitating activation. Although the molecular mechanism underlying Retigabine's action remains unknown, previous studies have identified the pore region of K...7 channels as the drug's target. This suggested that the Retigabine-induced shift in voltage dependence likely derives from the stabilization of the pore domain in an open (conducting) conformation. Testing this idea, we show that the heteromeric K...7.2/K...7.3 channel has at least two open states, which we named O... and O..., with O... being more stable. The O... state was reached after short membrane depolarizations, whereas O... was reached after prolonged depolarization or during steady state at the typical neuronal resting potentials. We also found that activation and deactivation seem to follow distinct pathways, suggesting that the K...7.2/K...7.3 channel activity displays hysteresis. As for the action of Retigabine, we discovered that this agonist discriminates between open states, preferentially acting on the O... state and further stabilizing it. Based on these findings, we proposed a novel mechanism for the therapeutic effect of Retigabine whereby this drug reduces excitability by enhancing the resting potential open state stability of K...7.2/K...7.3 channels. To address this hypothesis, we used a model for action potential (AP) in Xenopus laevis oocytes and found that the resting membrane potential became more negative as a function of Retigabine concentration, whereas the threshold potential for AP firing remained unaltered. (ProQuest: ... denotes formulae/symbols omitted.) |
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ISSN: | 0022-1295 1540-7748 |