Nitrendipine is a potent inhibitor of the Ca<sup>2+</sup>‐activated K<sup>+</sup> channel of human erythrocytes

Ellory, J. Clive; Kirk, Kiaran; Culliford, S.J.; Nash, Gerard B.; Stuart, J.

doi:10.1016/0014-5793(92)80383-r

Cited by 43 publications

(21 citation statements)

References 16 publications

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“…One pathway is the volume and pH-regulated K-Cl cotransport system (3,5). Though K-Cl cotransport activity is lower in the densest SS cells than in corresponding light and middle-density fractions, activity in these densest fractions is still higher than in AA inhibited by quinine, carbocyanine dyes (9), nifedipine (10), and nitrendipine ( 11) and with greater specificity by charybdotoxin (ChTX), a 37-amino acid peptide derived from the venom of Leiurus sequestratus (12)(13)(14). None of these drugs has been brought to clinical trial in sickle cell anemia, resulting either from low inhibitory potency (of the former) or from insufficient pharmacological specificity (of the latter) with expected attendant side effects.…”

Section: Introductionmentioning

confidence: 99%

Inhibition of Ca(2+)-dependent K+ transport and cell dehydration in sickle erythrocytes by clotrimazole and other imidazole derivatives.

Brugnara

Franceschi²,

Alper³

1993

J. Clin. Invest.

349

279

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We have investigated the interaction of clotrimazole (CLT) and related compounds with the erythroid Ca2"-activated K+ channel, a mediator of sickle cell dehydration. We measured K+ transport, membrane potential, and cell volume upon activation of this pathway in sickle erythrocytes. CLT blocked almost completely Ca2"-activated K+ transport in homozygous hemoglobin S cells, with IC5o values of 29±15 nM in isotonic 20 mM salt solution and 51±15 nM in normal saline (n = 3). The inhibition of K+ transport by CLT was caused by a specific interaction with the Ca2"-activated K+ channel of human red cells, since it displaced bound 125I-Charybdotoxin, a specific ligand of the Gardos channel, with an IC50 (12±4 nM in isotonic 20 mM) similar to the IC50 values for flux inhibition. When homozygous hemoglobin S cells were dehydrated by incubation in the presence of 100 ,gM CaCI2 and the ionophore A23187, or by exposure to cycles of oxygenation and deoxygenation, CLT effectively inhibited cell dehydration and K+ loss. The IC50 of CLT for inhibition of Ca2+-activated K+ transport in sickle cells is significantly lower than plasma concentrations of CLT achievable after nontoxic oral doses. We therefore propose that oral administration of CLT may prevent red cell dehydration in patients with sickle cell anemia. (J. Clin. Invest. 1993. 92:520-526.)

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Section: Introductionmentioning

confidence: 99%

Inhibition of Ca(2+)-dependent K+ transport and cell dehydration in sickle erythrocytes by clotrimazole and other imidazole derivatives.

Brugnara

Franceschi²,

Alper³

1993

J. Clin. Invest.

349

279

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“…In 86 Rb ϩ influx experiments cells were pretreated (for Ն10 min) with 0.1 mM ouabain to inhibit the Na ϩ /K ϩ pump, 0.01-0.1 mM bumetanide to inhibit the NaKCl 2 cotransporter, and 0.01-0.02 mM nitrendipine to inhibit the Ca 2ϩ -activated K ϩ channel (Ellory et al, 1992). In choline influx experiments the use of an extracellular choline concentration of 1 mM ensured that the endogenous erythrocyte choline carrier (which * This work was supported in part by Wellcome Trust Grants 036078/ Z/92/Z/1.5 and 041182/Z/94/Z and by the Lister Institute of Preventive Medicine.…”

Section: Materials-mentioning

confidence: 99%

Novel Anion Dependence of Induced Cation Transport in Malaria-infected Erythrocytes

Kirk

Horner

1995

Journal of Biological Chemistry

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Following invasion by the malaria parasite there appear in the parasitized erythrocyte new ("induced") permeation pathways that mediate the transport of a wide variety of small solutes. Although anion-selective, these pathways have a significant cation permeability and cause a substantial increase in the basal leak of cations into and out of the infected cell. In this study of human erythrocytes infected in vitro with Plasmodium falciparum it was shown that the transport of monovalent cations (Rb ؉ and choline), but not that of a nonelectrolyte (sorbitol) or a monovalent anion (lactate), via the malaria-induced pathways is strongly dependent on the nature of the anion in the suspending medium. Substitution of NO 3 ؊ for Cl ؊ resulted in a 4 -6-fold increase in the unidirectional influx and efflux of Rb Human erythrocytes infected with the mature (trophozoite) form of the malaria parasite, Plasmodium falciparum, show increased permeability to a diverse range of small solutes including polyols, amino acids, nucleosides, and monovalent anions and cations (reviewed by

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“…10,[17][18][19] It is also blocked by quinine, carbocyanine, nifedipine, and nitrendipine, although with low potency and/or specificity. [20][21][22][23] The human intermediate-conductance potassium channel (hIK1) was cloned in 1997 by scientists at Oregon Health Sciences University and Icagen. 19 The biophysical properties, pharmacology, and regulation of this Ca 2ϩ -activated K ϩ channel were determined to be indistinguishable from the RBC Gardos channel.…”

Section: Introductionmentioning

confidence: 99%

ICA-17043, a novel Gardos channel blocker, prevents sickled red blood cell dehydration in vitro and in vivo in SAD mice

Stocker

Franceschi

McNaughton‐Smith

et al. 2003

Blood

183

136

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Nitrendipine is a potent inhibitor of the Ca²⁺‐activated K⁺ channel of human erythrocytes

Cited by 43 publications

References 16 publications

Inhibition of Ca(2+)-dependent K+ transport and cell dehydration in sickle erythrocytes by clotrimazole and other imidazole derivatives.

Inhibition of Ca(2+)-dependent K+ transport and cell dehydration in sickle erythrocytes by clotrimazole and other imidazole derivatives.

Novel Anion Dependence of Induced Cation Transport in Malaria-infected Erythrocytes

ICA-17043, a novel Gardos channel blocker, prevents sickled red blood cell dehydration in vitro and in vivo in SAD mice

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Nitrendipine is a potent inhibitor of the Ca2+‐activated K+ channel of human erythrocytes

Cited by 43 publications

References 16 publications

Inhibition of Ca(2+)-dependent K+ transport and cell dehydration in sickle erythrocytes by clotrimazole and other imidazole derivatives.

Inhibition of Ca(2+)-dependent K+ transport and cell dehydration in sickle erythrocytes by clotrimazole and other imidazole derivatives.

Novel Anion Dependence of Induced Cation Transport in Malaria-infected Erythrocytes

ICA-17043, a novel Gardos channel blocker, prevents sickled red blood cell dehydration in vitro and in vivo in SAD mice

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Nitrendipine is a potent inhibitor of the Ca²⁺‐activated K⁺ channel of human erythrocytes