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MeSH: dovnitř usměrňující draslíkové kanály spřažené s G proteiny-metabolismus

3 záznamů v PubMed Filtry

Článek

The intriguing effect of ethanol and nicotine on acetylcholine-sensitive potassium current IKAch: Insight from a quantitative model

Šimurda, Jiří
Autor Šimurda, Jiří ORCID Department of Physiology, Faculty of Medicine, Masaryk University, Kamenice, Brno, Czech Republic
Šimurdová, Milena
Autor Šimurdová, Milena Department of Physiology, Faculty of Medicine, Masaryk University, Kamenice, Brno, Czech Republic
Bébarová, Markéta
Autor Bébarová, Markéta ORCID Department of Physiology, Faculty of Medicine, Masaryk University, Kamenice, Brno, Czech Republic

PloS one. 2019 ; 14 (10) : e0223448. [epub] 20191010

PLoS One
ISSN 1932-6203
Zdroj

Recent experimental work has revealed unusual features of the effect of certain drugs on cardiac inwardly rectifying potassium currents, including the constitutively active and acetylcholine-induced components of acetylcholine-sensitive current (IKAch). These unusual features have included alternating susceptibility of the current components to activation and inhibition induced by ethanol or nicotine applied at various concentrations, and significant correlation between the drug effect and the current magnitude measured under drug-free conditions. To explain these complex drug effects, we have developed a new type of quantitative model to offer a possible interpretation of the effect of ethanol and nicotine on the IKAch channels. The model is based on a description of IKAch as a sum of particular currents related to the populations of channels formed by identical assemblies of different α-subunits. Assuming two different channel populations in agreement with the two reported functional IKAch-channels (GIRK1/4 and GIRK4), the model was able to simulate all the above-mentioned characteristic features of drug-channel interactions and also the dispersion of the current measured in different cells. The formulation of our model equations allows the model to be incorporated easily into the existing integrative models of electrical activity of cardiac cells involving quantitative description of IKAch. We suppose that the model could also help make sense of certain observations related to the channels that do not show inward rectification. This new ionic channel model, based on a concept we call population type, may allow for the interpretation of complex interactions of drugs with ionic channels of various types, which cannot be done using the ionic channel models available so far.

MeSH
acetylcholin farmakologie MeSH
biologické modely MeSH
časové faktory MeSH
dovnitř usměrňující draslíkové kanály spřažené s G proteiny metabolismus MeSH
ethanol farmakologie MeSH
gating iontového kanálu účinky léků MeSH
nikotin farmakologie MeSH
počítačová simulace MeSH
Publikační typ
časopisecké články MeSH
práce podpořená grantem MeSH
Názvy látek
acetylcholin MeSH
dovnitř usměrňující draslíkové kanály spřažené s G proteiny MeSH
ethanol MeSH
nikotin MeSH

Článek

Effect of ethanol at clinically relevant concentrations on atrial inward rectifier potassium current sensitive to acetylcholine

Naunyn-Schmiedeberg's archives of pharmacology. 2016 Oct ; 389 (10) : 1049-58. [epub] 20160701

Naunyn Schmiedebergs Arch Pharmacol
ISSN 1432-1912 | 0028-1298
Zdroj

Alcohol intoxication tends to induce arrhythmias, most often the atrial fibrillation. To elucidate arrhythmogenic mechanisms related to alcohol consumption, the effect of ethanol on main components of the ionic membrane current is investigated step by step. Considering limited knowledge, we aimed to examine the effect of clinically relevant concentrations of ethanol (0.8-80 mM) on acetylcholine-sensitive inward rectifier potassium current I K(Ach). Experiments were performed by the whole-cell patch clamp technique at 23 ± 1 °C on isolated rat and guinea-pig atrial myocytes, and on expressed human Kir3.1/3.4 channels. Ethanol induced changes of I K(Ach) in the whole range of concentrations applied; the effect was not voltage dependent. The constitutively active component of I K(Ach) was significantly increased by ethanol with the maximum effect (an increase by ∼100 %) between 8 and 20 mM. The changes were comparable in rat and guinea-pig atrial myocytes and also in expressed human Kir3.1/3.4 channels (i.e., structural correlate of I K(Ach)). In the case of the acetylcholine-induced component of I K(Ach), a dual ethanol effect was apparent with a striking heterogeneity of changes in individual cells. The effect correlated with the current magnitude in control: the current was increased by eth-anol in the cells showing small current in control and vice versa. The average effect peaked at 20 mM ethanol (an increase of the current by ∼20 %). Observed changes of action potential duration agreed well with the voltage clamp data. Ethanol significantly affected both components of I K(Ach) even in concentrations corresponding to light alcohol consumption.

Klíčová slova
Dual effect, Ethanol, Inward rectifier, Kir3.1/3.4, Rat atrial cell model,
MeSH
acetylcholin farmakologie MeSH
akční potenciály MeSH
CHO buňky MeSH
Cricetulus MeSH
dovnitř usměrňující draslíkové kanály spřažené s G proteiny účinky léků genetika metabolismus MeSH
ethanol toxicita MeSH
hodnocení rizik MeSH
kardiomyocyty účinky léků metabolismus MeSH
kinetika MeSH
lidé MeSH
modely kardiovaskulární MeSH
morčata MeSH
počítačová simulace MeSH
potkani Wistar MeSH
srdeční arytmie chemicky indukované metabolismus patofyziologie MeSH
srdeční frekvence účinky léků MeSH
srdeční síně účinky léků metabolismus patofyziologie MeSH
transfekce MeSH
vztah mezi dávkou a účinkem léčiva MeSH
zvířata MeSH
Check Tag
lidé MeSH
morčata MeSH
mužské pohlaví MeSH
zvířata MeSH
Publikační typ
časopisecké články MeSH
Názvy látek
acetylcholin MeSH
dovnitř usměrňující draslíkové kanály spřažené s G proteiny MeSH
ethanol MeSH

Článek

Auxiliary GABAB receptor subunits uncouple G protein βγ subunits from effector channels to induce desensitization

Neuron. 2014 Jun 04 ; 82 (5) : 1032-44. [epub] 20140515

ISSN 1097-4199 | 0896-6273
Zdroj

Activation of K(+) channels by the G protein βγ subunits is an important signaling mechanism of G-protein-coupled receptors. Typically, receptor-activated K(+) currents desensitize in the sustained presence of agonists to avoid excessive effects on cellular activity. The auxiliary GABAB receptor subunit KCTD12 induces fast and pronounced desensitization of the K(+) current response. Using proteomic and electrophysiological approaches, we now show that KCTD12-induced desensitization results from a dual interaction with the G protein: constitutive binding stabilizes the heterotrimeric G protein at the receptor, whereas dynamic binding to the receptor-activated Gβγ subunits induces desensitization by uncoupling Gβγ from the effector K(+) channel. While receptor-free KCTD12 desensitizes K(+) currents activated by other GPCRs in vitro, native KCTD12 is exclusively associated with GABAB receptors. Accordingly, genetic ablation of KCTD12 specifically alters GABAB responses in the brain. Our results show that GABAB receptors are endowed with fast and reversible desensitization by harnessing KCTD12 that intercepts Gβγ signaling.

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