Human vascular to cardiac tissue selectivity of <scp>L</scp>‐ and <scp>T</scp>‐type calcium channel antagonists

Sarsero, Doreen; Fujiwara, Toshimasa; Molenaar, Peter; Angus, James A.

doi:10.1038/sj.bjp.0702045

Cited by 36 publications

(28 citation statements)

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“…Therefore, mibefradil may also have effects postjunctionally. For example, although these functional assays are sensitive to TTX (0.1 nM; neuronal Na + channel inhibitor), adrenoceptor antagonists and GVIA (N-type VOCC selective; Pruneau and Angus 1990), mibefradil at 30 µM also inhibited postjunctional calcium channels opened by exogenous isoprenaline in human isolated atria muscle (Sarsero et al 1998).…”

Section: Discussionmentioning

confidence: 99%

“…This 15-fold or so selectivity is exhibited by its potency (IC 50 ) to inhibit the T-type calcium currents in cloned (α1G, 0.27 µM and α1H, 0.14 µM with 2.0 mM Ca 2+ as charge carrier; Martin et al 2000) and native T-type Ca 2+ currents (rat vascular smooth muscle 0.2 µM; Mishra and Hermsmeyer 1994) at lower concentrations than required to inhibit L-type calcium currents (α1C from 1.7 µM to 21 µM, rat vascular smooth muscle 2.6 µM; Mehrke et al 1994;Mishra and Hermsmeyer 1994;Bezprozvanny and Tsien 1995;Seisenberger et al 1995;Welling et al 1995;Martin et al 2000). Some effects of mibefradil that may be due to T-type VOCC inhibition include: the selectivity for vascular relaxation over negative cardiac inotropism (Osterrieder and Holck 1989;Brixius et al 1998;Sarsero et al 1998), reduction in heart rate (Ertel et al 1997), reduction in subendothelial cell proliferation (Schmitt et al 1995(Schmitt et al , 1996, and protective benefits in hypertension and animals with heart failure (Bernink et al 1996;Davies et al 1997;Li and Schiffrin 1997;Massie et al 1997;Oparil et al 1997;Hermsmeyer 1998;Clozel et al 1999;Sandmann et al 2001). Although mibefradil has been withdrawn from therapy by the manufacturer because of interactions with other drugs (Griffin 1998;Krahenbuhl et al 1998;Mullins et al 1998;Spoendlin et al 1998), the therapeutic benefits of mibefradil were considered to be mainly due to the blockade of T-type VOCCs.…”

Section: Introductionmentioning

confidence: 99%

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Evidence against an action of mibefradil at N-type voltage-operated calcium channels

Angus

2001

Naunyn-Schmiedeberg's Archives of Pharmacology

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Mibefradil is a tetralol derivative that inhibits cloned and native T-type voltage-operated calcium channels (VOCCs) at an IC50 of 1 microM and with an apparent 15-fold selectivity for T- over L-type VOCCs. Recent electrophysiological studies in Xenopus oocytes and inhibition of noradrenaline release studies in human isolated right atria concluded that mibefradil (0.3-3 microM) can block N-type VOCCs like omega-conotoxin GVIA. We tested this hypothesis in rat and guinea pig isolated driven left atria and rat vas deferens in response to sympathetic nerve stimulation. Mibefradil (3 microM) did not inhibit the inotropic responses to sympathetic electrical field stimulation in atria. In contrast, these responses were blocked by GVIA (10 nM) and tetrodotoxin (TTX 0.1 microM). In rat vas deferens, pretreated with benextramine (BNX 10 microM), contractions considered to be due to transmitter ATP evoked by electrical field stimulation were blocked by: (a) TTX 0.1 microM, (b) P2x receptor desensitisation (alphabeta-MeATP 100 microM), and (c) GVIA (pIC50 9.04+/-0.15, n=5). In contrast, mibefradil (0.3-30 microM) had no effect on these N-type VOCC-sensitive sympathetic nerve responses. Potassium (62 mM K+) and alphabeta-MeATP-induced contractions were unaffected by GVIA (10 nM), but mibefradil inhibited the potassium-induced contractions with a pIC50 6.02+/-0.08 (n=5), consistent with a T- and L-type VOCC blocking action on the postjunctional smooth muscle. We conclude that mibefradil up to 30 microM does not block N-type VOCCs in these isolated intact tissue assays of sympathetic nerve-muscle transmission. Therefore, at least in these tissues, mibefradil can be used to define T- and L-type VOCC activities at submicromolar and micromolar concentrations in sympathetic nerve-mediated responses.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Evidence against an action of mibefradil at N-type voltage-operated calcium channels

Angus

2001

Naunyn-Schmiedeberg's Archives of Pharmacology

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“…Mibefradil increased CF with an EC 50 of 54 nM and reduced contractility of myocardium and aorta with EC 50 values of 14 µM and 275 nM, respectively [337]. In human small arteries, the potassium contractures and isoprenaline-stimulated right atrial contractions were inhibited with IC 50 values of 603 nM and 24.5 µM, respectively, indicating a high (41) vascular selectivity of mibefradil [8]. 300 and 600 nM mibefradil showed a marked vascular selectivity in Langendorff-perfused rat hearts [334].…”

Section: Mibefradil (Ro 40-5967) Animal Studies With Mibefradilmentioning

confidence: 94%

Class IV Antiarrhythmic Agents: New Compounds Using an Old Strategy

Szentandrássy

Nagy²,

Hegyi³

et al. 2014

CPD

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Cardiac arrhythmias are a major cause of morbidity and mortality in the industrialized world. Among their treatment regimens one can find the calcium channel antagonists (CCAs), the class IV agents. In the cardiovascular system Land T-type calcium channels are found on vascular smooth muscle cells and cardiac myocytes with well defined physiological roles. Inhibition of calcium channels by CCAs has widely been used in clinical practice for several decades. Cardiovascular disorders are one of the many fields of medicine in which CCAs are used for various reasons and conditions. The three main indications of them are hypertension, angina and various cardiac arrhythmias. The most important classes of CCAs are dihydropyridines, phenylalkylamines and benzothiazepines but some newer compounds do not fall into any of these major classes. Dihydropyridines are not used in the antiarrhythmic therapy but are good vasodilators and antianginal agents. In contrast, phenylalkylamines and benzothiazepines exert cardiac actions in vivo and therefore these are one choice of antiarrhythmic drugs. This review focuses on phenylalkylamines, benzothiazepines and on new drugs with potential antiarrhythmic action in the heart as well as the mechanisms how calcium channels antagonism can lead to an antiarrhythmic action.

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“…The inotropic potency of verapamil was 1/3 of its vasodilator potency; this ratio was 1/17 for nifedipine, and less than 1/800 for efonidipine. In isolated human or rat tissues the vascular (as compared to cardiac) selectivity was higher for mibefradil than for other Ca 2+ channel blockers that acted mainly on L-type Ca 2+ channels (47). The extremely low negative inotropic potency of efonidipine may also involve additional mechanisms such as enhancement of Ca 2+ sensitivity of myocardial contractile proteins (27).…”

Section: Fig 3 Effects Of Efonidipine Nifedipine and Nimentioning

confidence: 97%

Efonidipine Hydrochloride: A Dual Blocker of L‐ and T‐Type Ca²⁺ Channels

Tanaka

Shigenobu

2002

Cardiovascular Drug Reviews

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T-type Ca 2+ channels have properties different from those of the L-type and are involved in cardiac pacemaking and regulation of blood flow, but not in myocardial contraction. Efonidipine is an antihypertensive and antianginal drug with dihydropyridine structure that was recently found to block both L-and T-type Ca 2+ channels. In isolated myocardial and vascular preparations, efonidipine has potent negative chronotropic and vasodilator effects but only a weak negative inotropic effect. In experimental animals and patients, reduction of blood pressure by the drug was accompanied by no or minimum reflex tachycardia leading to improvement of myocardial oxygen balance and maintenance of cardiac output. Efonidipine increased glomerular filtration rate without increasing intraglomerular pressure. By relaxing both the afferent and efferent arterioles, efonidipine markedly reduced proteinuria. Thus, efonidipine, an L-and T-type dual Ca 2+ channel blocker, appears to have an ideal profile as an antihypertensive and antianginal drug with organ-protective effects in the heart and kidney.

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Human vascular to cardiac tissue selectivity of L‐ and T‐type calcium channel antagonists

Cited by 36 publications

References 36 publications

Evidence against an action of mibefradil at N-type voltage-operated calcium channels

Evidence against an action of mibefradil at N-type voltage-operated calcium channels

Class IV Antiarrhythmic Agents: New Compounds Using an Old Strategy

Efonidipine Hydrochloride: A Dual Blocker of L‐ and T‐Type Ca²⁺ Channels

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Human vascular to cardiac tissue selectivity of L‐ and T‐type calcium channel antagonists

Cited by 36 publications

References 36 publications

Evidence against an action of mibefradil at N-type voltage-operated calcium channels

Evidence against an action of mibefradil at N-type voltage-operated calcium channels

Class IV Antiarrhythmic Agents: New Compounds Using an Old Strategy

Efonidipine Hydrochloride: A Dual Blocker of L‐ and T‐Type Ca2+ Channels

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Efonidipine Hydrochloride: A Dual Blocker of L‐ and T‐Type Ca²⁺ Channels