Evaluation of the bronchodilator properties of Ro 31–6930, a novel potassium channel opener, in the guinea‐pig

Paciorek, P.M.; Cowlrick, Ivor; Perkins, Rosie; Taylor, John; Wilkinson, Gary; Waterfall, J.F.

doi:10.1111/j.1476-5381.1990.tb15797.x

Cited by 42 publications

(14 citation statements)

References 23 publications

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“…In the present study, the IC50 of levcromakalim was in agreement with other reports using vascular and airway smooth muscle [9,[26][27][28][29]; it was more potent than THEO. However, levcromakalim cannot be a first-line regimen for bronchodilatation, since the β-adrenergic agonist, ISO, was much more potent than levcromakalim in this study.…”

Section: Discussionsupporting

confidence: 82%

“…However, levcromakalim cannot be a first-line regimen for bronchodilatation, since the β-adrenergic agonist, ISO, was much more potent than levcromakalim in this study. The relationship between the three bronchodilators, β-adrenergic agonist, KATP openers and THEO supports the results reported by PACIOREK et al [27], where the order of guinea-pig tracheal relaxants was always salbutamol > Ro 31-6930 (a potassium channel opener) > cromakalim > THEO.…”

Section: Discussionsupporting

confidence: 79%

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Allergic responses reduce the relaxant effect of beta-agonists but not potassium channel openers in guinea-pig isolated trachea

Houjou¹,

Iizuka²,

Dobashi³

et al. 1996

Eur Respir J

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This study was conducted to determine whether the relaxant effect of adenosine triphosphate (ATP)-sensitive potassium channel (KATP) openers on airway smooth muscle are reduced during the hyporesponsiveness of beta-adrenergic receptors. Isometric tension was measured and dose-response curves were constructed for levcromakalim (a KATP opener), Y-26763 (another KATP opener), isoprenaline and theophylline in guinea-pig isolated trachea that was challenged with ovalbumin or pretreated in vitro with either isoprenaline or the KATP openers. Antigen challenge in vitro significantly reduced the potency but not the efficacy of isoprenaline in tracheal strips from actively sensitized guinea-pigs. The concentration of drug that produced a half-maximum inhibition (IC50) was 0.014 +/- 0.004 microM in the challenge group versus 0.006 +/- 0.001 microM in the control group (p < 0.05; n = 9). The IC50 of levcromakalim (1.73 +/- 0.17 microM; n = 6) and of theophylline (110 +/- 3.1 microM; n = 6) were unaffected. Exposure to 4 microM isoprenaline for 30 min evoked beta-adrenergic hyporesponsiveness: the IC50 of isoprenaline rose significantly from 0.010 +/- 0.001 to 0.017 +/- 0.002 microM (p < 0.01; n = 6). No effect was observed on the relaxant actions of levcromakalim and theophylline. In contrast, prior incubation with either levcromakalim or Y-26763 (300 microM for 30 min) significantly reduced the subsequent potency and efficacy of levcromakalim, but did not alter the effects of isoprenaline and theophylline. We conclude that the relaxant effect of the adenosine triphosphate-sensitive potassium channel openers was independent of beta-adrenergic hyporesponsiveness in airway smooth muscle of guinea-pigs.

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Section: Discussionsupporting

confidence: 82%

Section: Discussionsupporting

confidence: 79%

Allergic responses reduce the relaxant effect of beta-agonists but not potassium channel openers in guinea-pig isolated trachea

Houjou¹,

Iizuka²,

Dobashi³

et al. 1996

Eur Respir J

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“…Distribution of KC 128-sensitive K+ channel in various airway tissues Generally, ATP-sensitive K+ channel openers, including levcromakalim, have been reported to be not very effective on cholinoceptor agonist-induced contraction in the guinea-pig tracheal smooth muscle (Allen et al, 1986;Nielsen-Kudsk et al, 1988;Paciorek et al, 1990;Taylor et al, 1992;Imagawa et al, 1993). It has also been reported that the relaxant effects of K+ channel openers in airway tissues were largely dependent on the concentration of agonist used (Raeburn & Brown, 1991).…”

Section: Discussionmentioning

confidence: 99%

Regional and species differences in glyburide‐sensitive K⁺ channels in airway smooth muscles as estimated from actions of KC 128 and levcromakalim

Kamei¹,

Yoshida²,

Imagawa³

et al. 1994

British J Pharmacology

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1 The purpose of the present experiments was to elucidate the differences in actions of two K+ channel openers, KC 128 and levcromakalim, on the carbachol-induced contraction, membrane potential and 86Rb+ efflux of the dog tracheal and bronchial smooth muscles. Furthermore, we compared the effects of these agents on guinea-pig and human airway smooth muscles. 2 In the dog tracheal and bronchial smooth muscle tissues, levcromakalim induced a concentrationdependent relaxation of the carbachol-induced contraction. The IC50 values were 0.35 AM (pIC5: 6.46 ± 0.10, n = 9) and 0.55 JM (pIC5o: 6.26 ± 0.07, n = 5), respectively. KC 128 relaxed bronchial smooth muscles precontracted by carbachol with an IC50 value of 0.19 AIM (pICG0: 6.73 ± 0.10, n = 7).However, KC 128 had almost no effect on the contraction evoked by carbachol in the trachea (ICGo> 10 0tM). The relaxations induced by levcromakalim and KC 128 were antagonized by glyburide (0.03-1 gM) but not by charybdotoxin (100 nM). 3 Levcromakalim (1 gM) hyperpolarized the membrane of both dog tracheal and bronchial smooth muscle cells, whereas KC 128 (1 tM) hyperpolarized the membrane of bronchial but not of tracheal smooth muscle cells.4 Levcromakalim (10 g.M) increased 'Rb+ efflux rate from both tracheal and bronchial smooth muscle tissues but KC 128 (10 gM) increased 86Rb+ efflux rate only from bronchial and not tracheal smooth muscle tissues. Glyburide (1 tM) prevented the hyperpolarization and the 'Rb+ efflux induced by these agents at the same concentration as observed for mechanical responses. 5Both KC 128 and levcromakalim relaxed the guinea-pig isolated tracheal smooth muscles precontracted by carbachol (100 nM), histamine (3 gM) or U46619 (10 nM). KC 128 was approximately 10 times more potent than levcromakalim for each agonist. 6 In human bronchial smooth muscles, levcromakalim but not KC 128 induced a concentrationdependent relaxation of the carbachol-induced contraction. 7 It is concluded that KC 128 has relaxant and hyperpolarizing effects in the dog bronchial and guinea-pig tracheal smooth muscles, but not in the dog tracheal and human bronchial smooth muscles. On the other hand, levcromakalim acts consistently on all the above airway smooth muscle tissues. These results indicate that there are regional and species differences in distribution of K+ channels, and at least two different K+ channel opener-and glyburide-sensitive K+ channels are present in the dog airway smooth muscles.

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“…The effects of potassium channel openers in suppressing the tone of airway smooth muscle in vitro are well established (Allen et al, 1986;Bray et al, 1987;Arch et al, 1988;NielsenKudsk et al, 1988;Paciorek et al, 1990;Berry et al, 1991;Raeburn & Brown, 1991). The effects of potassium channel openers on neurally-mediated responses in the airways have also attracted interest.…”

Section: Introductionmentioning

confidence: 99%

Effects of cromakalim on neurally‐mediated responses of guinea‐pig tracheal smooth muscle

Burka

Berry

Foster

et al. 1991

British J Pharmacology

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1 The ability of cromakalim to modulate several different types of neuroeffector transmission has been assessed in guinea-pig isolated trachea. 2 In trachea treated with propranolol (10-6M) and indomethacin (2.8 x 10-6M), stimulation of the extrinsic vagal nerves evoked contractions which were blocked by hexamethonium (5 x 10-4M) or by tetrodotoxin (TTX; 10-6M). Cromakalim (10-'M) caused a two fold rightward shift of the frequencyresponse curve.3 In carinal trachea treated with propranolol and indomethacin, transmural stimulation evoked an initial, rapid contraction followed by a more sustained secondary contraction. The initial, rapid contractile response was virtually ablated by atropine (10-6 M) or by TTX but was resistant to hexamethonium. Cromakalim (10-8-10-M) caused a concentration-dependent rightward shift of the frequency-response curve for the initial contraction. 4 In carinal trachea treated with atropine, propranolol and indomethacin, transmural stimulation evoked only the secondary (non-adrenergic, non-cholinergic (NANC)) contractile responses. These were markedly reduced by TTX but were resistant to hexamethonium. Cromakalim (10-8-10-5M) suppressed the NANC contractile responses in a concentration-dependent manner. This action could be offset by glibenclamide (10-6M). 5 In trachea treated with atropine, histamine (10-4M), propranolol and indomethacin, transmural stimulation evoked NANC relaxant responses. Cromakalim (up to 10-5 M) was without effect on the frequencyresponse curve for the stimulation of NANC inhibitory nerves. 6 Tested on trachea bathed by drug-free Krebs solution, cromakalim (10--1O-5M) caused concentration-dependent suppression of tracheal tone. In trachea treated with propranolol and indomethacin, cromakalim (10-7-1O-5 M) caused concentration-dependent antagonism of acetylcholine (ACh). In trachea treated with atropine, propranolol and indomethacin, cromakalim (up to 10-5M) failed to antagonize effects of either histamine or substance P. 7 It is concluded that cromakalim can inhibit cholinergic (excitatory) neuroeffector transmission in the trachea but only at a concentration having demonstrable inhibitory activity against the action of exogenous ACh and the spontaneous tone of the airways smooth muscle. In contrast, cromakalim may depress NANC excitatory (putative peptidergic) neuroeffector transmission at a concentration below that exerting inhibitory activity on airways smooth muscle. Cromakalim does not concurrently depress NANC inhibitory neuroeffector transmission. Depression of NANC excitatory neuroeffector transmission could explain the ability of cromakalim to suppress airway hyperreactivity or bronchial asthma at doses lacking direct relaxant effect on airways smooth muscle.

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Evaluation of the bronchodilator properties of Ro 31–6930, a novel potassium channel opener, in the guinea‐pig

Cited by 42 publications

References 23 publications

Allergic responses reduce the relaxant effect of beta-agonists but not potassium channel openers in guinea-pig isolated trachea

Allergic responses reduce the relaxant effect of beta-agonists but not potassium channel openers in guinea-pig isolated trachea

Regional and species differences in glyburide‐sensitive K⁺ channels in airway smooth muscles as estimated from actions of KC 128 and levcromakalim

Effects of cromakalim on neurally‐mediated responses of guinea‐pig tracheal smooth muscle

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Evaluation of the bronchodilator properties of Ro 31–6930, a novel potassium channel opener, in the guinea‐pig

Cited by 42 publications

References 23 publications

Allergic responses reduce the relaxant effect of beta-agonists but not potassium channel openers in guinea-pig isolated trachea

Allergic responses reduce the relaxant effect of beta-agonists but not potassium channel openers in guinea-pig isolated trachea

Regional and species differences in glyburide‐sensitive K+ channels in airway smooth muscles as estimated from actions of KC 128 and levcromakalim

Effects of cromakalim on neurally‐mediated responses of guinea‐pig tracheal smooth muscle

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Regional and species differences in glyburide‐sensitive K⁺ channels in airway smooth muscles as estimated from actions of KC 128 and levcromakalim