External Ba2+ Block of the Two-pore Domain Potassium Channel TREK-1 Defines Conformational Transition in Its Selectivity Filter

Ma, Xiaoyun; Yu, Jin-Mei; Zhang, Shuzhuo; Liu, Xiaoyan; Wu, Baohong; Wei, Xiaoli; Yan, Jiaqing; Sun, Hongjian; Yan, Hang; Zheng, Jimin

doi:10.1074/jbc.m111.264788

Cited by 43 publications

(54 citation statements)

References 43 publications

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“…The alternative translation initiation codon is 42 amino acids upstream from the first methionine in the sequence at the N-terminus of the channel. The N-terminus truncated form gives rise to a current with a much reduced open probability and a collapsed selectivity filter with both a reduced potassium selectivity [61,74,94,100] and a measurable permeability to sodium [94]. Treatment with both DEPC and fenamates, substantially enhances current through the Nterminus truncated form of the channel, and, interestingly, measurements of the reversal potential in the presence of these compounds reveal that the enhanced currents have become highly K selective [99,100].…”

Section: Fenamatesmentioning

confidence: 94%

Two-pore domain potassium channels: potential therapeutic targets for the treatment of pain

Mathie

Veale

2014

Pflugers Arch - Eur J Physiol

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Recent evidence points to a pivotal contribution of a variety of different potassium channels, including two-pore domain potassium (K2P) channels, in chronic pain processing. Expression of several different K2P channel subunits has been detected in nociceptive dorsal root ganglion neurons and trigeminal ganglion neurons, in particular, TREK1, TREK2, TRESK, TRAAK, TASK3 and TWIK1 channels. Of these, the strongest body of evidence from functional studies highlights the importance of TREK1, TRESK and, recently, TREK2 channels. For example, TREK1 knockout mice are more sensitive than wild-type mice to a number of painful stimuli but less sensitive to morphine-induced analgesia. TRESK knockdown mice show behavioural evidence of increased pain and increased sensitivity to painful pressure. Importantly, familial migraine with aura is associated with a dominant-negative mutation in human TRESK channels. Thus, the functional up-regulation of K2P channel activity may be a useful strategy in the development of new therapies for the treatment of pain. Whilst there are few currently available compounds that selectively and directly enhance the activity of TRESK and TREK2 channels, recent advances have been made in terms of identifying compounds that activate TREK1 channels and in understanding how they might act on the channel. Large-scale bio-informatic approaches and the further development of databases of putative ligands, channel structures and putative ligand binding sites on these structures may form the basis for future experimental strategies to detect novel molecules acting to enhance K2P channel activity that would be useful in the treatment of pain.

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Section: Fenamatesmentioning

confidence: 94%

Two-pore domain potassium channels: potential therapeutic targets for the treatment of pain

Mathie

Veale

2014

Pflugers Arch - Eur J Physiol

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“…Thomas et al (2008) describe the N terminus truncated form of TREK1 (TREK1DN) as being regionally and developmentally regulated in a number of different regions of the rat central nervous system. Both forms are expressed in COS-7 cells (Thomas et al, 2008) but predominantly the long form is found in human embryonic kidney 293 cells (Ma et al, 2011). For the related K2P channel TREK2, which also undergoes ATI (Simkin et al, 2008), the degree of ATI has been shown to be tissue specific (Staudacher et al, 2011) through differential regulation of mRNA translation.…”

Section: N Terminus Modulates Trek1 Channel Pharmacologymentioning

confidence: 99%

“…TREK1DN has been described as a constitutively "nonconductive" variant, with a "collapsed selectivity filter" (Ma et al, 2011) that is permeable to sodium under normal physiologic conditions, leading to membrane depolarization when it is active in neurons (Thomas et al, 2008). Furthermore, TREK1DN has been shown to copurify with the longer form (Thomas et al, 2008), so heteromers may also exist.…”

Section: N Terminus Modulates Trek1 Channel Pharmacologymentioning

confidence: 99%

Influence of the N Terminus on the Biophysical Properties and Pharmacology of TREK1 Potassium Channels

et al. 2014

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TWIK-related K 1 1 (TREK1) potassium channels are members of the two-pore domain potassium channel family and contribute to background potassium conductances in many cell types, where their activity can be regulated by a variety of physiologic and pharmacologic mediators. amine] enhance the activity of TREK1 currents, and we show that BL-1249 is the most potent of these compounds. Alternative translation initiation produces a shorter, N terminus truncated form of TREK1 with a much reduced open probability and a proposed increased permeability to sodium compared with the longer form. We show that both forms of TREK1 can be activated by fenamates and that a number of mutations that affect TREK1 channel gating occlude the action of fenamates but only in the longer form of TREK1. Furthermore, fenamates produce a marked enhancement of current through the shorter, truncated form of TREK1 and reveal a K 1 -selective channel, like the long form. These results provide insight into the mechanism of TREK1 channel activation by fenamates, and, given the role of TREK1 channels in pain, they suggest a novel analgesic mechanism for these compounds.

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“…[5]. However, we have very limited information about its possible effect on background leak channels [26], or on cardiac Ca 2+ activated K + channels. Therefore, we should not assign the significant Ca 2+ sensitivity of I K1 to a single channel type.…”

Section: Multifactor Regulation Of I K1 ?mentioning

confidence: 99%

[Ca2+]i-induced augmentation of the inward rectifier potassium current (IK1) in canine and human ventricular myocardium

Nagy

Acsai

Kormos

et al. 2013

Pflugers Arch - Eur J Physiol

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External Ba2+ Block of the Two-pore Domain Potassium Channel TREK-1 Defines Conformational Transition in Its Selectivity Filter

Cited by 43 publications

References 43 publications

Two-pore domain potassium channels: potential therapeutic targets for the treatment of pain

Two-pore domain potassium channels: potential therapeutic targets for the treatment of pain

Influence of the N Terminus on the Biophysical Properties and Pharmacology of TREK1 Potassium Channels

[Ca2+]i-induced augmentation of the inward rectifier potassium current (IK1) in canine and human ventricular myocardium

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