Closing and Inactivation Potentiate the Cocaethylene Inhibition of Cardiac Sodium Channels by Distinct Mechanisms

O’Leary, Michael E.; Digregorio, M.; Chahine, Mohamed

doi:10.1124/mol.64.6.1575

Cited by 13 publications

(14 citation statements)

References 41 publications

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“…Two highly conserved aromatic amino acids (F1760 and Y1767) of DIVS6 are known to be critical determinants of drug binding (40). The Y1767C mutation examined in this study is known to weaken the anesthetic inhibition of Na v 1.5 channels, consistent with an important role for this residue in drug binding (36,37). The data show that class I antiarrhythmic drugs (quinidine, mexiletine, lidocaine, and flecainide) are relatively weak inhibitors of the Y1767C-induced persistent Na ϩ current (Fig.…”

Section: Discussionmentioning

confidence: 52%

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Y1767C, a novel SCN5A mutation, induces a persistent Na⁺ current and potentiates ranolazine inhibition of Na_v1.5 channels

Huang

Priori

Napolitano

et al. 2011

American Journal of Physiology-Heart and Circulatory Physiology

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Long QT syndrome type 3 (LQT3) has been traced to mutations of the cardiac Na+ channel (Nav1.5) that produce persistent Na+ currents leading to delayed ventricular repolarization and torsades de pointes. We performed mutational analyses of patients suffering from LQTS and characterized the biophysical properties of the mutations that we uncovered. One LQT3 patient carried a mutation in the SCN5A gene in which the cysteine was substituted for a highly conserved tyrosine (Y1767C) located near the cytoplasmic entrance of the Nav1.5 channel pore. The wild-type and mutant channels were transiently expressed in tsA201 cells, and Na+ currents were recorded using the patch-clamp technique. The Y1767C channel produced a persistent Na+ current, more rapid inactivation, faster recovery from inactivation, and an increased window current. The persistent Na+ current of the Y1767C channel was blocked by ranolazine but not by many class I antiarrhythmic drugs. The incomplete inactivation, along with the persistent activation of Na+ channels caused by an overlap of voltage-dependent activation and inactivation, known as window currents, appeared to contribute to the LQTS phenotype in this patient. The blocking effect of ranolazine on the persistent Na+ current suggested that ranolazine may be an effective therapeutic treatment for patients with this mutation. Our data also revealed the unique role for the Y1767 residue in inactivating and forming the intracellular pore of the Nav1.5 channel.

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Section: Discussionmentioning

confidence: 52%

“…Y1767 is situated near the cytoplasmic end of the DIVS6 segment and is an important determinant of antiarrhythmic drug binding (36,37). The aromatic side chain at this position appears to be exposed within the aqueous pore, where it is believed to directly interact with bound drugs (1).…”

Section: Discussionmentioning

confidence: 99%

Y1767C, a novel SCN5A mutation, induces a persistent Na⁺ current and potentiates ranolazine inhibition of Na_v1.5 channels

Huang

Priori

Napolitano

et al. 2011

American Journal of Physiology-Heart and Circulatory Physiology

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“…Mutation I 4i11 A in the muscle and brain Na ϩ channels makes them sensitive to extracellularly applied quaternary LAs (Ragsdale et al, 1994;Wang et al, 1998;Sunami et al, 2001). Furthermore, mutation I 4i11 C facilitates escape of the trapped cocaethylene from Na v 1.5 (O'Leary et al, 2003). Our models explain the effects of these mutations: the bulky Ile 4i11 in the wild type Na v 1.4 prevents LAs to enter the pore, whereas smaller Ala 4i11 enables LAs to pass.…”

Section: I22mentioning

confidence: 62%

“…External QX-222 increased block of the I 4i11 A Na v 1.4 mutant in the presence of the -CTX mutant R13N, suggesting that the outer pore is not the access route for the LA . Furthermore, the mutation I 4i11 C in Na v 1.5 enhanced binding and facilitated escape of cocaethylene from the closed channel (O'Leary et al, 2003).…”

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confidence: 99%

Access and Binding of Local Anesthetics in the Closed Sodium Channel

Bruhova

Tikhonov²,

Zhorov

2008

Molecular Pharmacology

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Local anesthetics (LAs) are known to bind Na ϩ channels in the closed, open, and inactivated states and reach their binding sites via extracellular and intracellular access pathways. Despite intensive studies, no atomic-scale theory is available to explain the diverse experimental data on the LA actions. Here we attempt to contribute to this theory by simulating access and binding of LAs in the KcsA-based homology model of the closed Na ϩ channel. We used Monte Carlo minimizations to model the channel with representative local anesthetics N-(2,6-dimethylphenylcarbamoylmethyl)triethylammonium (QX-314), cocaine, and tetracaine. We found the nucleophilic central cavity to be a common binding region for the ammonium group of LAs, whose aromatic group can extend either along the pore axis (vertical binding mode) or to the III/IV domain interface (horizontal binding mode). The vertical mode was earlier predicted for the open channel, but only the horizontal mode is consistent with mutational data on the closed-channel block.

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“…The latter is completely impermeant to cell membranes and needs to be applied intracellularly to reach its receptor and inhibit sodium currents. The substitution of an isoleucine residue in the extracellular third of D4S6 (I1760 in rat Nav1.2, I1575 in rat Nav1.4; I1756 in human Nav1.5) with alanine, cysteine or glutamate was shown to create an external access pathway, thereby allowing QX314 to block sodium channels from the outside and facilitate LA drug escape from the closed channel (Ragsdale et al, 1994;Wang et al, 1998;Sunami et al, 2001;O'Leary et al, 2003). In contrast to other isoforms, the cardiac Nav1.5 channel is blocked by external QX314, and replacement of threonine 1765 in rNav1.5 by valine, which is a native residue in rNav1.2 reduced this block (Qu et al, 1995); conversely, a cysteine mutation to threonine at this site in rNav1.4 creates an external access for QX314 (Sunami et al, 2000).…”

Section: J-f Desaphy Et Almentioning

confidence: 99%

Molecular determinants of state‐dependent block of voltage‐gated sodium channels by pilsicainide

Desaphy

Dipalma

Costanza

et al. 2010

British J Pharmacology

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Background and purpose: Pilsicainide, an anti-arrhythmic drug used in Japan, is described as a pure sodium channel blocker. We examined the mechanisms by which it is able to block open channels, because these properties may be especially useful to reduce hyperexcitability in pathologies characterized by abnormal sodium channel opening. Experimental approach: The effects of pilsicainide on various heterologously expressed human sodium channel subtypes and mutants were investigated using the patch clamp technique. Key results: Pilsicainide exhibited tonic and use-dependent effects comparable to those of mexiletine and flecainide on hNav1.4 channels. These use-dependent effects were abolished in the mutations F1586C and Y1593C within segment 6 of domain IV, suggesting that the interaction of pilsicainide with these residues is critical for its local anaesthetic action. Its affinity constants for closed channels (KR) and channels inactivated from the closed state (KI) were high, suggesting that its use-dependent block (UDB) requires the channel to be open for it to reach a high-affinity blocking site. Accordingly, basic pH, which slightly increased the proportion of neutral drug, dramatically decreased KR and KI values. Effects of pilsicainide were similar on skeletal muscle hNav1.4, brain hNav1.1 and heart hNav1.5 channels. The myotonic R1448C and G1306E hNav1.4 mutants were more and less sensitive to pilsicainide, respectively, due to mutation-induced gating modifications. Conclusions and implications:Although therapeutic concentrations of pilsicainide may have little effect on resting and closed-state inactivated channels, it induces a strong UDB due to channel opening, rendering the drug ideally suited for inhibition of high-frequency action potential firing. Abbreviations: h and (1 -h), proportions of closed and inactivated channels at a particular potential; ICTRL, peak current amplitude measured in the same cell before drug application; IDRUG, peak current amplitude measured in the presence of drug; INa, whole-cell sodium current; KAPP, apparent affinity constant at a given potential; KI, affinity for inactivated channels; KR, affinity for closed channels; LA, local anaesthetic; S, slope factor; TB, tonic block; UDB, use-dependent block; V, conditioning pulse potential; V1/2, half-maximum inactivation potential British Journal of Pharmacology IntroductionDue to their ability to act as sodium channel blockers, local anaesthetic (LA)-like drugs can be used to treat a large spectrum of disorders including cardiac arrhythmias, epilepsy, myotonia and neuropathic pain (Conte Camerino et al., 2007). Many of these drugs present a tertiary amine associated with a hydrophobic aromatic tail through an amide, ester or ether link. The two ends of the drug may interact with channel pore-lining amino acids through hydrophobic or p-cation interactions (Ragsdale et al., 1994;Wright et al., 1998;Nau et al., 1999;Wang et al., 2000;Yarov-Yarovoy et al., 2001;O'Leary and Chahine, 2002;McNulty et al., 2007;Ahern et al., 2008;Sunam...

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Closing and Inactivation Potentiate the Cocaethylene Inhibition of Cardiac Sodium Channels by Distinct Mechanisms

Cited by 13 publications

References 41 publications

Y1767C, a novel SCN5A mutation, induces a persistent Na⁺ current and potentiates ranolazine inhibition of Na_v1.5 channels

Y1767C, a novel SCN5A mutation, induces a persistent Na⁺ current and potentiates ranolazine inhibition of Na_v1.5 channels

Access and Binding of Local Anesthetics in the Closed Sodium Channel

Molecular determinants of state‐dependent block of voltage‐gated sodium channels by pilsicainide

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Closing and Inactivation Potentiate the Cocaethylene Inhibition of Cardiac Sodium Channels by Distinct Mechanisms

Cited by 13 publications

References 41 publications

Y1767C, a novel SCN5A mutation, induces a persistent Na+ current and potentiates ranolazine inhibition of Nav1.5 channels

Y1767C, a novel SCN5A mutation, induces a persistent Na+ current and potentiates ranolazine inhibition of Nav1.5 channels

Access and Binding of Local Anesthetics in the Closed Sodium Channel

Molecular determinants of state‐dependent block of voltage‐gated sodium channels by pilsicainide

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Y1767C, a novel SCN5A mutation, induces a persistent Na⁺ current and potentiates ranolazine inhibition of Na_v1.5 channels

Y1767C, a novel SCN5A mutation, induces a persistent Na⁺ current and potentiates ranolazine inhibition of Na_v1.5 channels