On the mechanism of isoprenaline‐ and forskolin‐induced depolarization of single guinea‐pig ventricular myocytes.

Egan, Terrance M.; Noble, Denis; Noble, S J; Powell, T.; Twist, V. W.; Yamaoka, Kaoru

doi:10.1113/jphysiol.1988.sp017121

Cited by 71 publications

(78 citation statements)

References 37 publications

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“…The observed hyperpolarization of the membrane potential, V., by isoprenaline in skeletal muscle fibres, has been attributed to stimulation of the Na+-K+-pump by the cyclic AMPdependent cascade (Clausen, 1986;Li & Sperelakis, 1993). From the literature on cardiac tissue however, a more complex picture emerges comprising influences on V. by the stimulation of the Na+-K+-pump (D1silets & Baumgarten, 1986), K+-conductance (Gadsby, 1983;Boyden et al, 1983a), Na+-conductance (Egan et al, 1988), Ca2+-conductance (Tsien et al, 1986) or Cl--conductance (Harvey & Hume, 1989;Ehara & Ishihara, 1990;Nakaya et al, 1990). Also combinations of these effects have been proposed (Encina et al, 1988;Harvey et al, 1991).…”

Section: Introductionmentioning

confidence: 99%

Modulation of the isoprenaline‐induced membrane hyperpolarization of mouse skeletal muscle cells

Mil

Kerkhof

Heukelom

1995

British J Pharmacology

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1 The hyperpolarization of the resting membrane potential, V., induced by isoprenaline in the lumbrical muscle fibres of the mouse, was investigated by use of intracellular microelectrodes.2 In normal Krebs-Henseleit solution (potassium concentration: K+= 5.7 mM, 'control'), V. was -74.0±0.2 mV; lowering K+ to 0.76 mM ('low K'7) resulted in either a hyperpolarization (VM -95.7± 2.9 mV), or a depolarization (Vm= -52.0± 0.3 mV). When Vm hyperpolarized after switching to low K', the addition of isoprenaline resulted in increased hyperpolarization Vm: AVm=-16.3 + 3.2 mV to a final Vm=-110.1I±3.4 mV. Adding iso-prenaline when Vm depolarized in low K+, leads to a hyperpolarization of either by -11.6 ± 0.5 mV to -63.6+0.8 mV or by -51.7+2.7 mV to -106.9±3.9 mV. 5 Ouabain (0.1 to 1 mM) did not suppress the hyperpolarization by isoprenaline in 5.7 mM K + (AVm=-6.7±0.4 mV) or the hyperpolarization of the depolarized cells in low K + (AVm= 9.7 ±1.5 mV). 6The hyperpolarization is a logarithmically decreasing function of K + in the range between 2 and 20 mM (12 mV/decade). 7 IBMX and 8Br-cyclic AMP mimicked the response to isoprenaline whereas forskolin (FSK) induced in low K + a hyperpolarization of -7.0±0.7 mV that could be augmented by addition of isoprenaline (AVm -8.2± 1.8 mV). 8In control and low K+, Ba2`(0.6 mM) inhibited the hyperpolarization induced by isoprenaline, IBMX or 8Br-cyclic AMP. Other blockers of the potassium conductance such as TEA (5 mM) and apamin (0.4 riM) had no effect. 9 We conclude that in the lumbrical muscle of the mouse the isoprenaline-induced hyperpolarization is primarily due to an increase in potassium permeability.

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Section: Introductionmentioning

confidence: 99%

Modulation of the isoprenaline‐induced membrane hyperpolarization of mouse skeletal muscle cells

Mil

Kerkhof

Heukelom

1995

British J Pharmacology

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“…It is likely that adenosine antagonism of catecholamine stimulated increases in ICa resulted from effects on intracellular cyclic AMP levels (Lerman & Belardinelli, 1990). These actions of adenosine are mediated through adenosine Al receptors coupled to the catalytic subunit of adenylyl cyclase through a pertussis toxin-sensitive guanine nucleotide binding regulatory (Ga) protein (Belardinelli & Pelleg, 1990 (Egan et al, 1988;Boachie-Ansah et al, 1993). It has been suggested that activation of catecholamine induced currents could generate an ectopic ventricular focus leading to tachycardia.…”

Section: Discussionmentioning

confidence: 99%

“…It has been suggested that activation of catecholamine induced currents could generate an ectopic ventricular focus leading to tachycardia. If more than one focus were activated asynchronously then the rhythm could become chaotic and might precipitate ventricular fibrillation (Egan et al, 1988). Accordingly, subcutaneous administration of isoprenaline was used to facilitate ventricular fibrillation in vivo.…”

Section: Discussionmentioning

confidence: 99%

Antiarrhythmic effects of BN‐063, a newly synthesized adenosine A₁ agonist, on myocardial ischaemia in rats

Lee

Chern

Yen

1994

British J Pharmacology

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It has been shown that adenosine is able to reduce the severity of arrhythmias induced by myocardial ischaemia. In isolated preparations, the antiarrhythmic effect of adenosine on ventricular myocardium is known to antagonize the catecholamine‐induced stimulation of intracellular cyclic AMP production, an effect mediated via adenosine A1 receptors. The aim of this study was to evaluate the antiarrhythmic effect of BN‐063 (1‐cyclo‐propylisoguanosine), a newly synthesized selective adenosine A1 agonist, on ventricular arrhythmias in rats. Arrhythmias were induced by left coronary artery ligation or by administration of isoprenaline (7 mg kg−1) subcutaneously. Pretreatment with BN‐063 (0.25, 0.5 and 1.0 mg kg−1) 10 min prior to occlusion significantly delayed the onset of ventricular arrhythmias, reduced the total number of ventricular premature contraction (VPC) and ventricular tachycardia (VT), decreased the incidence of VT and ventricular fibrillation (VF) and mortality during the first 30 min following left coronary artery ligation. In contrast, pretreatment with 8‐cyclopentyl‐1,3‐dipropylxanthine (DPCPX), an adenosine A1 antagonist, was arrhythmogenic during the ischaemic period. The rate‐pressure product, an index for indirect measurement of myocardial oxygen consumption, was also significantly reduced by BN‐063 during ligation time. The incidence of VT, VF and mortality was also significantly reduced when BN‐063 was administered after left coronary artery ligation. BN‐063 converted the VF induced by isoprenaline to normal sinus rhythm and improved the survival rate. It is concluded that, through activation of adenosine A1 receptors, BN‐063 can suppress ventricular arrhythmias induced by myocardial ischaemia and catecholamines. The antiarrhythmic actions of BN‐063 may be mediated by reducing heart rate and antagonizing the stimulatory effects of catecholamine in myocardial ischaemia.

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“…A variety of potentially important C1-currents have been described in the heart, and they are suggested to play pathophysiological roles by modulating the excitability of cardiac myocyte [1][2][3][4][5][6][7][8][9]. Membrane depolarization induced by a PKAactivated C1-current may result in development of severe arrhythmias associated with acute myocardial infarction [1][2][3].…”

Section: Introductionmentioning

confidence: 99%

“…Membrane depolarization induced by a PKAactivated C1-current may result in development of severe arrhythmias associated with acute myocardial infarction [1][2][3]. A swelling-induced C1-current contributes to the pacemaker potential in sino-atrial nodal cells, and activation of this current results in acceleration of cardiac heart rate [7,8].…”

Section: Introductionmentioning

confidence: 99%

Molecular cloning and characterization of a novel truncated form (ClC‐2β) of ClC‐2α (ClC‐2G) in rabbit heart

et al. 1995

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Two cDNAs encoding rabbit heart CI-channels (rahCIC-21~l and rabCIC-2c0 were isolated by a PCR cloning strategy. RabCIC-21~l is a novel cDNA consisting of 2998 bp and encoding the 822-amino acid protein, while rabCIC-2a is identical to previously reported CIC-2G. RabCIC-2/] is 68 amino acids truncated from NHz-terminus of rabCIC-2a, but aH 13 putative hydrophobic domains are conserved in rabCIC-2/3. Although rabCIC-2a was suggested to be activated by extracellular hypotonicity, expression of rabCIC-2/3 in Xenopus oocytes induced large Cl-currents even in the absence of extracellular hypotonicity. Induction of external hypotonicity did not further increase the amplitude of membrane currents. On the other hand, as similar to rabCIC-2a, rabCIC-21~ current was augmented by PKA activation. Thus, different RNA processing of the same gene appears to provide two highly homologous PKA-activated CIchannels with or without responsiveness to cell swelling in rabbit heart.

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On the mechanism of isoprenaline‐ and forskolin‐induced depolarization of single guinea‐pig ventricular myocytes.

Cited by 71 publications

References 37 publications

Modulation of the isoprenaline‐induced membrane hyperpolarization of mouse skeletal muscle cells

Modulation of the isoprenaline‐induced membrane hyperpolarization of mouse skeletal muscle cells

Antiarrhythmic effects of BN‐063, a newly synthesized adenosine A₁ agonist, on myocardial ischaemia in rats

Molecular cloning and characterization of a novel truncated form (ClC‐2β) of ClC‐2α (ClC‐2G) in rabbit heart

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On the mechanism of isoprenaline‐ and forskolin‐induced depolarization of single guinea‐pig ventricular myocytes.

Cited by 71 publications

References 37 publications

Modulation of the isoprenaline‐induced membrane hyperpolarization of mouse skeletal muscle cells

Modulation of the isoprenaline‐induced membrane hyperpolarization of mouse skeletal muscle cells

Antiarrhythmic effects of BN‐063, a newly synthesized adenosine A1 agonist, on myocardial ischaemia in rats

Molecular cloning and characterization of a novel truncated form (ClC‐2β) of ClC‐2α (ClC‐2G) in rabbit heart

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Antiarrhythmic effects of BN‐063, a newly synthesized adenosine A₁ agonist, on myocardial ischaemia in rats