Differential Activation of Vascular Smooth Muscle Kv7.4, Kv7.5, and Kv7.4/7.5 Channels by ML213 and ICA-069673

Brueggemann, Lyubov I.; Haick, Jennifer M.; Cribbs, Leanne L.; Byron, Kenneth L.

doi:10.1124/mol.114.093799

Cited by 47 publications

(61 citation statements)

References 51 publications

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“…4B); a slight suppression of the current observed in the presence of rolipram was not statistically significant. Subsequent application of the nonselective Kv7.2-Kv7.5 activator ML213 (10 mM) (Yu et al, 2011;Brueggemann et al, 2014a) robustly enhanced the MASMC Kv7 currents and this effect was reversed by the selective Kv7 channel blocker XE991 (10 mM) (Fig. 4B), demonstrating the expected pharmacological characteristics of the Kv7 currents and confirming our ability to detect an increase in current amplitude in these cells.…”

Section: Kt5720supporting

confidence: 72%

“…4). A7r5 cells natively express only Kv7.5 channels (Brueggemann et al, 2007, whereas MASMCs predominantly express Kv7.4/Kv7.5 channels (Brueggemann et al, , 2014a. Insensitivity of MASMC Kv7.4/7.5 channels to rolipram was replicated when this same subunit combination was expressed in A7r5 cells, suggesting that the difference in regulation of native Kv7 currents between A7r5 cells and MASMCs relates primarily to the Kv7 channel subunit stoichiometry rather than to differences in PDE isoforms (Polson and Strada, 1996;Dunkerley et al, 2002;Maurice et al, 2003).…”

Section: Discussionmentioning

confidence: 96%

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Kv7.5 Potassium Channel Subunits Are the Primary Targets for PKA-Dependent Enhancement of Vascular Smooth Muscle Kv7 Currents

et al. 2015

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Kv7 (KCNQ) channels, formed as homo-or heterotetramers of Kv7.4 and Kv7.5 a-subunits, are important regulators of vascular smooth muscle cell (VSMC) membrane voltage. Recent studies demonstrate that direct pharmacological modulation of VSMC Kv7 channel activity can influence blood vessel contractility and diameter. However, the physiologic regulation of Kv7 channel activity is still poorly understood. Here, we study the effect of cAMP/protein kinase A (PKA) activation on whole cell K 1 currents through endogenous Kv7.5 channels in A7r5 rat aortic smooth muscle cells or through Kv7.4/Kv7.5 heteromeric channels natively expressed in rat mesenteric artery smooth muscle cells. The contributions of specific a-subunits are further dissected using exogenously expressed human Kv7.4 and Kv7.5 homo-or heterotetrameric channels in A7r5 cells. Stimulation of Ga scoupled b-adrenergic receptors with isoproterenol induced PKA-dependent activation of endogenous Kv7.5 currents in A7r5 cells. The receptor-mediated enhancement of Kv7.5 currents was mimicked by pharmacological agents that increase [cAMP] (forskolin, rolipram, 3-isobutyl-1-methylxanthine, and papaverine) or mimic cAMP (8-bromo-cAMP); the 2-to 4-fold PKA-dependent enhancement of currents was also observed with exogenously expressed Kv7.5 channels. In contrast, exogenously-expressed heterotetrameric Kv7.4/7.5 channels in A7r5 cells or native mesenteric artery smooth muscle Kv7.4/7.5 channels were only modestly enhanced, and homo-tetrameric Kv7.4 channels were insensitive to this regulatory pathway. Correspondingly, proximity ligation assays indicated that isoproterenol induced PKAdependent phosphorylation of exogenously expressed Kv7.5 channel subunits, but not of Kv7.4 subunits. These results suggest that signal transduction-mediated responsiveness of vascular smooth muscle Kv7 channel subunits to cAMP/PKA activation follows the order of Kv7.5 .. Kv7.4/Kv7.5 . Kv7.4.

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Section: Kt5720supporting

confidence: 72%

Section: Discussionmentioning

confidence: 96%

Kv7.5 Potassium Channel Subunits Are the Primary Targets for PKA-Dependent Enhancement of Vascular Smooth Muscle Kv7 Currents

et al. 2015

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“…Although it is less potent than its related analog ICA-27243, ICA-069673 displays greater efficacy and improved selectivity for heteromeric K V 7.2/K V 7.3 over K V 7.1 channels (Amato et al, 2011). In contrast with retigabine, which binds to the pore region (S5 to S6) of K V 7.2-K V 7.5 channels (Gunthorpe et al, 2012), evidence suggests that ICA-069673 is among an emerging novel class of compounds known as "gating modifiers," named so for their ability to bind to the S1-S4 voltage-sensing domain of K V 7 channels Peretz et al, 2010;Brueggemann et al, 2014a).…”

Section: Discussionmentioning

confidence: 99%

“…ICA-069673 did not affect K V 7.1 channels, which are predominately expressed in the heart (Amato et al, 2011). A recent study on A7r5 smooth muscle cells demonstrated that ICA-069673 was effective in activating recombinantly expressed K V 7.4 channels (Brueggemann et al, 2014a). However, K V 7.4 channel protein expression was not observed in guinea pig DSM (Afeli et al, 2013).…”

Section: Introductionmentioning

confidence: 86%

The Novel K_V7.2/K_V7.3 Channel Opener ICA-069673 Reveals Subtype-Specific Functional Roles in Guinea Pig Detrusor Smooth Muscle Excitability and Contractility

Provence

Malysz

Petkov

2015

J Pharmacol Exp Ther

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The physiologic roles of voltage-gated K V 7 channel subtypes (K V 7.1-K V 7.5) in detrusor smooth muscle (DSM) are poorly understood. Here, we sought to elucidate the functional roles of K V 7.2/K V 7.3 channels in guinea pig DSM excitability and contractility using the novelWe employed a multilevel experimental approach using Western blot analysis, immunocytochemistry, isometric DSM tension recordings, fluorescence Ca 21 imaging, and perforated whole-cell patch-clamp electrophysiology. Western blot experiments revealed the protein expression of K V 7.2 and K V 7.3 channel subunits in DSM tissue. In isolated DSM cells, immunocytochemistry with confocal microscopy further confirmed protein expression for K V 7.2 and K V 7.3 channel subunits, where they localize within the vicinity of the cell membrane. ICA-069673 inhibited spontaneous phasic, pharmacologically induced, and nerve-evoked contractions in DSM isolated strips in a concentration-dependent manner. The inhibitory effects of ICA-069673 on DSM spontaneous phasic and tonic contractions were abolished in the presence of the K V 7 channel inhibitor XE991 [10,10-bis(4-pyridinylmethyl)-9 (10H)-anthracenone dihydrochloride]. Under conditions of elevated extracellular K 1 (60 mM), the effects of ICA-069673 on DSM tonic contractions were significantly attenuated. ICA-069673 decreased the global intracellular Ca 21 concentration in DSM cells, an effect blocked by the L-type Ca 21 channel inhibitor nifedipine. ICA-069673 hyperpolarized the membrane potential and inhibited spontaneous action potentials of isolated DSM cells, effects that were blocked in the presence of XE991. In conclusion, using the novel K V 7.2/ K V 7.3 channel activator ICA-069673, this study provides strong evidence for a critical role for the K V 7.2-and K V 7.3-containing channels in DSM function at both cellular and tissue levels.

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“…; Brueggemann et al . ). Several studies have suggested the possibility that certain KCNQ activators may act on a distinct site present in certain KCNQ subtypes.…”

Section: Introductionmentioning

confidence: 97%

Sequence determinants of subtype‐specific actions of KCNQ channel openers

Wang

Yang

Kurata

2016

The Journal of Physiology

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Retigabine (RTG) is the first approved anti-epileptic drug that acts via activation of voltage-gated potassium channels, targeting KCNQ channels that underlie the neuronal M-current. RTG exhibits little specificity between KCNQ2-5 as a result of conservation of a Trp residue in the pore domain that binds to the drug. The RTG analogue ICA-069673 ('ICA73') exhibits much stronger effects on KCNQ2 channels, including a large hyperpolarizing shift of the voltage-dependence of activation, an ∼2-fold enhancement of peak current and pronounced subtype specificity for KCNQ2 over KCNQ3. Based on ICA73 sensitivity of chimeric constructs of the transmembrane segments of KCNQ2 and KCNQ3, this drug appears to interact with the KCNQ2 voltage sensor (S1-S4) rather than the pore region targeted by RTG. KCNQ2 point mutants in the voltage sensor were generated based on KCNQ2/KCNQ3 sequence differences, and screened for ICA73 sensitivity. These experiments reveal that KCNQ2 residues F168 and A181 in the S3 segment are essential determinants of ICA73 subtype specificity. Mutations at either position in KCNQ2 abolish the ICA73-mediated gating shift, but preserve RTG sensitivity. Interestingly, A181P mutant channels show little ICA73-mediated gating shift but retain current potentiation by the drug. Mutations (L198F and P211A), which introduce these critical KCNQ2 residues at corresponding positions in KCNQ3, transplant partial ICA73 sensitivity. These findings demonstrate that RTG and ICA73 act via distinct mechanisms, and also reveal specific residues that underlie subtype specificity of KCNQ channel openers.

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Differential Activation of Vascular Smooth Muscle Kv7.4, Kv7.5, and Kv7.4/7.5 Channels by ML213 and ICA-069673

Cited by 47 publications

References 51 publications

Kv7.5 Potassium Channel Subunits Are the Primary Targets for PKA-Dependent Enhancement of Vascular Smooth Muscle Kv7 Currents

Kv7.5 Potassium Channel Subunits Are the Primary Targets for PKA-Dependent Enhancement of Vascular Smooth Muscle Kv7 Currents

The Novel K_V7.2/K_V7.3 Channel Opener ICA-069673 Reveals Subtype-Specific Functional Roles in Guinea Pig Detrusor Smooth Muscle Excitability and Contractility

Sequence determinants of subtype‐specific actions of KCNQ channel openers

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Differential Activation of Vascular Smooth Muscle Kv7.4, Kv7.5, and Kv7.4/7.5 Channels by ML213 and ICA-069673

Cited by 47 publications

References 51 publications

Kv7.5 Potassium Channel Subunits Are the Primary Targets for PKA-Dependent Enhancement of Vascular Smooth Muscle Kv7 Currents

Kv7.5 Potassium Channel Subunits Are the Primary Targets for PKA-Dependent Enhancement of Vascular Smooth Muscle Kv7 Currents

The Novel KV7.2/KV7.3 Channel Opener ICA-069673 Reveals Subtype-Specific Functional Roles in Guinea Pig Detrusor Smooth Muscle Excitability and Contractility

Sequence determinants of subtype‐specific actions of KCNQ channel openers

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The Novel K_V7.2/K_V7.3 Channel Opener ICA-069673 Reveals Subtype-Specific Functional Roles in Guinea Pig Detrusor Smooth Muscle Excitability and Contractility