Detrusor Smooth Muscle KV7 Channels: Emerging New Regulators of Urinary Bladder Function

Malysz, John; Petkov, Georgi V.

doi:10.3389/fphys.2020.01004

Cited by 7 publications

(4 citation statements)

References 99 publications

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“…It is worth noting that different types of smooth muscle cells, including smooth myocytes of the urinary bladder, have been demonstrated to be functionally expressed in the activity of K M (KCNQx) channels [52,53,[78][79][80][81][82][83][84][85][86][87][88][89]. The SOL-induced interaction with K M channels to modify the magnitude and gating of I K(M) has the propensity to change muscarinic cholinergic activation involved in the micturition reflex, presuming that the in vivo results happen.…”

Section: Discussionmentioning

confidence: 99%

The Effectiveness in Activating M-Type K+ Current Produced by Solifenacin ([(3R)-1-azabicyclo[2.2.2]octan-3-yl] (1S)-1-phenyl-3,4-dihydro-1H-isoquinoline-2-carboxylate): Independent of Its Antimuscarinic Action

Cho

Chuang

2021

IJMS

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Solifenacin (Vesicare®, SOL), known to be a member of isoquinolines, is a muscarinic antagonist that has anticholinergic effect, and it has been beneficial in treating urinary incontinence and neurogenic detrusor overactivity. However, the information regarding the effects of SOL on membrane ionic currents is largely uncertain, despite its clinically wide use in patients with those disorders. In this study, the whole-cell current recordings revealed that upon membrane depolarization in pituitary GH3 cells, the exposure to SOL concentration-dependently increased the amplitude of M-type K+ current (IK(M)) with effective EC50 value of 0.34 μM. The activation time constant of IK(M) was concurrently shortened in the SOL presence, hence yielding the KD value of 0.55 μM based on minimal reaction scheme. As cells were exposed to SOL, the steady-state activation curve of IK(M) was shifted along the voltage axis to the left with no change in the gating charge of the current. Upon an isosceles-triangular ramp pulse, the hysteretic area of IK(M) was increased by adding SOL. As cells were continually exposed to SOL, further application of acetylcholine (1 μM) failed to modify SOL-stimulated IK(M); however, subsequent addition of thyrotropin releasing hormone (TRH, 1 μM) was able to counteract SOL-induced increase in IK(M) amplitude. In cell-attached single-channel current recordings, bath addition of SOL led to an increase in the activity of M-type K+ (KM) channels with no change in the single channel conductance; the mean open time of the channel became lengthened. In whole-cell current-clamp recordings, the SOL application reduced the firing of action potentials (APs) in GH3 cells; however, either subsequent addition of TRH or linopirdine was able to reverse SOL-mediated decrease in AP firing. In hippocampal mHippoE-14 neurons, the IK(M) was also stimulated by adding SOL. Altogether, findings from this study disclosed for the first time the effectiveness of SOL in interacting with KM channels and hence in stimulating IK(M) in electrically excitable cells, and this noticeable action appears to be independent of its antagonistic activity on the canonical binding to muscarinic receptors expressed in GH3 or mHippoE-14 cells.

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Section: Discussionmentioning

confidence: 99%

The Effectiveness in Activating M-Type K+ Current Produced by Solifenacin ([(3R)-1-azabicyclo[2.2.2]octan-3-yl] (1S)-1-phenyl-3,4-dihydro-1H-isoquinoline-2-carboxylate): Independent of Its Antimuscarinic Action

Cho

Chuang

2021

IJMS

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“…This possible adverse event should be monitored in future studies: voltage-gated K+ channels regulate the bladder detrusor smooth muscle function and ezogabine-produced urinary retention in rodents but had minimal effects in humans. 18 At baseline, the subject's median seizure frequency was ~13 per month (28 days). 16,17 During the study treatment, participants in the 25 mg, 20 mg, 10 mg and placebo groups had a median percentage change in monthly seizure frequency of 52.8%, 46.4%, 33.3% and 18.2%, respectively.…”

Section: Xen1101 Clinical Trials: Preliminary Resultsmentioning

confidence: 99%

XEN1101: A Novel Potassium Channel Modulator for the Potential Treatment of Focal Epilepsy in Adults

Krauss¹

2022

Neurology

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Antiseizure medications that reduce seizures via new mechanisms are needed. XEN1101 is an agonist of voltage-gated potassium ion channels (Kv) that was recently shown to reduce focal-onset seizures in a placebo-controlled phase II study. The molecular structure of this potassium channel “opener” is different from ezogabine/retigabine, preventing dimer formation and the pigmentary deposition associated with ezogabine/retigabine treatment. This article reviews the pharmacology and early clinical results for XEN1101.

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“…Although K V 7.2 and K V 7.3 subunits are mainly expressed in the nervous system, K V 7.4 and K V 7.5 are also abundantly expressed in non-neuronal tissues. In fact, K V 7.4 and K V 7.5 are the major K V 7 subunits in smooth muscles of vasculature and hollow visceral organs where they regulate the smooth muscle contractility and vascular tone (Jepps et al, 2013;Malysz and Petkov, 2020), and in skeletal muscle where they regulate the proliferation, differentiation and muscle force development (Schroeder et al, 2000;Iannotti et al, 2013;Zagorchev et al, 2016). Opening K V 7.4 or K V 7.4/7.5 channels in these tissues likely contributes to the common side effects of retigabine, such as urinary retention, asthenia and symptomatic hypotension.…”

Section: Introductionmentioning

confidence: 99%

Selective KCNQ2/3 Potassium Channel Opener ICA-069673 Inhibits Excitability in Mouse Vagal Sensory Neurons

Sun,

Undem

2024

J Pharmacol Exp Ther

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Heightened excitability of vagal sensory neurons in inflammatory visceral diseases contributes to unproductive and difficult-to-treat neuronally based symptoms such as visceral pain and dysfunction. Identification of targets and modulators capable of regulating the excitability of vagal sensory neurons may lead to novel therapeutic options. KCNQ1-5 genes encode K V 7.1-7.5 potassium channel α-subunits. Homotetrameric or heterotetrameric K V 7.2-7.5 channels can generate the so-called M-current (I M ) known to decrease the excitability of neurons including visceral sensory neurons. This study aimed to address the hypothesis that K V 7.2/7.3 channels are key regulators of vagal sensory neuron excitability by evaluating the effects of KCNQ2/3selective activator, ICA-069673, on I M in mouse nodose neurons and determining its effects on excitability and action potential firings using patch clamp technique. The results showed that ICA-069673 enhanced I M density, accelerated the activation and delayed the deactivation of Mchannels in a concentration-dependent manner. ICA-069673 negatively shifted the voltagedependent activation of I M and increased the maximal conductance. Consistent with its effects on I M , ICA-069673 induced a marked hyperpolarization of resting potential and reduced the input resistance. The hyperpolarizing effect was more pronounced in partially depolarized neurons.Moreover, ICA-069673 caused a 3-fold increase in the minimal amount of depolarizing current needed to evoke an action potential, and significantly limited the action potential firings in response to sustained suprathreshold stimulations. ICA-069673 had no effect on membrane currents when Kcnq2 and Kcnq3 were deleted. These results indicate that opening KCNQ2/3mediated M-channels is sufficient to suppress the excitability and enhance spike accommodation in vagal visceral sensory neurons.

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Detrusor Smooth Muscle KV7 Channels: Emerging New Regulators of Urinary Bladder Function

Cited by 7 publications

References 99 publications

The Effectiveness in Activating M-Type K+ Current Produced by Solifenacin ([(3R)-1-azabicyclo[2.2.2]octan-3-yl] (1S)-1-phenyl-3,4-dihydro-1H-isoquinoline-2-carboxylate): Independent of Its Antimuscarinic Action

The Effectiveness in Activating M-Type K+ Current Produced by Solifenacin ([(3R)-1-azabicyclo[2.2.2]octan-3-yl] (1S)-1-phenyl-3,4-dihydro-1H-isoquinoline-2-carboxylate): Independent of Its Antimuscarinic Action

XEN1101: A Novel Potassium Channel Modulator for the Potential Treatment of Focal Epilepsy in Adults

Selective KCNQ2/3 Potassium Channel Opener ICA-069673 Inhibits Excitability in Mouse Vagal Sensory Neurons

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