Literature DB >> 7811912

Amine blockers of the cytoplasmic mouth of sodium channels: a small structural change can abolish voltage dependence.

G W Zamponi1, R J French.   

Abstract

Many drugs block sodium channels from the cytoplasmic end (Moczydlowski, E., A. Uehara, X, Guo, and J. Heiny. 1986. Isochannels and blocking modes of voltage-dependent sodium channels. Ann. N.Y. Acad. Sci. 479:269-292.). Lidocaine, applied to either side of the membrane, induces two blocking modes, a rapid, voltage-dependent open-channel block, and a block of the inactivated channel that occurs on a 1000-fold slower timescale. Here we describe the actions of several lidocaine-related amines on batrachotoxin(BTX)-activated bovine cardiac sodium channels incorporated into planar lipid bilayers. We applied blocking amines from the intracellular side and examined the structural determinants of fast, open-channel block. Neither hydroxyl nor carbonyl groups, present in the aryl-amine link of lidocaine, were necessary, indicating that hydrogen bonding between structures in the aryl-amine link and the channel is not required. Block, however, was significantly enhanced by addition of an aromatic ring, or by the lengthening of aliphatic side chains, suggesting that a hydrophobic domain strengthens binding while the amine group blocks the pore. For most blockers, depolarizing potentials enhanced block, with the charged amine group apparently traversing 45-60% of the transmembrane voltage. By contrast, block by phenylhydrazine was essentially voltage-independent. The relatively rigid planar structure of phenylhydrazine may prevent the charged amino end from entering the electric field when the aromatic ring is bound. The relation between structural features of different blockers and their sensitivity to voltage suggests that the transmembrane voltage drops completely over less than 5 A. We raise the possibility that the proposed hydrophobic binding domain overlaps the endogenous receptor for the inactivation gate. If so, our data place limits on the distance between this receptor and the intrapore site at which charged amines bind.

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Year:  1994        PMID: 7811912      PMCID: PMC1225454          DOI: 10.1016/S0006-3495(94)80567-3

Source DB:  PubMed          Journal:  Biophys J        ISSN: 0006-3495            Impact factor:   4.033


  35 in total

1.  Sodium currents in voltage clamped nerve fiber of frog under the combined action of batrachotoxin and procaine.

Authors:  B I Khodorov; E M Peganov; S V Revenko; L D Shishkova
Journal:  Brain Res       Date:  1975-02-14       Impact factor: 3.252

2.  Block of single batrachotoxin-activated Na+ channels by clofilium.

Authors:  J Nettleton; N A Castle; G K Wang
Journal:  Mol Pharmacol       Date:  1991-03       Impact factor: 4.436

3.  The effect of tetramethylammonium on single sodium channel currents.

Authors:  R Horn; J Patlak; C F Stevens
Journal:  Biophys J       Date:  1981-11       Impact factor: 4.033

4.  Quantifying antiarrhythmic drug blocking during action potentials in guinea-pig papillary muscle.

Authors:  K R Courtney
Journal:  J Mol Cell Cardiol       Date:  1983-11       Impact factor: 5.000

5.  Interval-dependent effects of small antiarrhythmic drugs on excitability of guinea-pig myocardium.

Authors:  K R Courtney
Journal:  J Mol Cell Cardiol       Date:  1980-11       Impact factor: 5.000

6.  Further analysis of the mechanisms of action of batrachotoxin on the membrane of myelinated nerve.

Authors:  B I Khodorov; S V Revenko
Journal:  Neuroscience       Date:  1979       Impact factor: 3.590

7.  Aminoalkyl structural requirements for interaction of lidocaine with the class I antiarrhythmic drug receptor on rat cardiac myocytes.

Authors:  R S Sheldon; R J Hill; M Taouis; L M Wilson
Journal:  Mol Pharmacol       Date:  1991-05       Impact factor: 4.436

8.  Tetramethylammonium ions alter sodium-channel gating in Myxicola.

Authors:  C L Schauf
Journal:  Biophys J       Date:  1983-03       Impact factor: 4.033

9.  Single sodium channels from rat brain incorporated into planar lipid bilayer membranes.

Authors:  B K Krueger; J F Worley; R J French
Journal:  Nature       Date:  1983 May 12-18       Impact factor: 49.962

10.  Ion permeation in normal and batrachotoxin-modified Na+ channels in the squid giant axon.

Authors:  A M Correa; R Latorre; F Bezanilla
Journal:  J Gen Physiol       Date:  1991-03       Impact factor: 4.086
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  11 in total

1.  Tetrapentylammonium block of chloramine-T and veratridine modified rat brain type IIA sodium channels.

Authors:  A S Ghatpande; S Rao; S K Sikdar
Journal:  Br J Pharmacol       Date:  2001-04       Impact factor: 8.739

2.  Block of voltage-operated sodium channels by 2,6-dimethylphenol, a structural analogue of lidocaine's aromatic tail.

Authors:  Gertrud Haeseler; Johannes Bufler; Sarah Merken; Reinhard Dengler; Jeffrey Aronson; Martin Leuwer
Journal:  Br J Pharmacol       Date:  2002-09       Impact factor: 8.739

3.  Locations of local anesthetic dibucaine in model membranes and the interaction between dibucaine and a Na+ channel inactivation gate peptide as studied by 2H- and 1H-NMR spectroscopies.

Authors:  Y Kuroda; M Ogawa; H Nasu; M Terashima; M Kasahara; Y Kiyama; M Wakita; Y Fujiwara; N Fujii; T Nakagawa
Journal:  Biophys J       Date:  1996-09       Impact factor: 4.033

4.  Sodium current inhibition by internal calcium: a combination of open-channel block and surface charge screening?

Authors:  G W Zamponi; R J French
Journal:  J Membr Biol       Date:  1995-09       Impact factor: 1.843

5.  Trans-channel interactions in batrachotoxin-modified rat skeletal muscle sodium channels: kinetic analysis of mutual inhibition between mu-conotoxin GIIIA derivatives and amine blockers.

Authors:  Quanli Ma; Evgeny Pavlov; Tatiana Britvina; Gerald W Zamponi; Robert J French
Journal:  Biophys J       Date:  2008-07-25       Impact factor: 4.033

6.  Trans-channel interactions in batrachotoxin-modified skeletal muscle sodium channels: voltage-dependent block by cytoplasmic amines, and the influence of mu-conotoxin GIIIA derivatives and permeant ions.

Authors:  Evgeny Pavlov; Tatiana Britvina; Jeff R McArthur; Quanli Ma; Iván Sierralta; Gerald W Zamponi; Robert J French
Journal:  Biophys J       Date:  2008-07-25       Impact factor: 4.033

7.  Molecular basis of ranolazine block of LQT-3 mutant sodium channels: evidence for site of action.

Authors:  Sandra Fredj; Kevin J Sampson; Huajun Liu; Robert S Kass
Journal:  Br J Pharmacol       Date:  2006-05       Impact factor: 8.739

8.  Increased hindrance on the chiral carbon atom of mexiletine enhances the block of rat skeletal muscle Na+ channels in a model of myotonia induced by ATX.

Authors:  J F Desaphy; D Conte Camerino; C Franchini; G Lentini; V Tortorella; A De Luca
Journal:  Br J Pharmacol       Date:  1999-11       Impact factor: 8.739

9.  Classification of drugs based on properties of sodium channel inhibition: a comparative automated patch-clamp study.

Authors:  Nora Lenkey; Robert Karoly; Peter Lukacs; E Sylvester Vizi; Morten Sunesen; Laszlo Fodor; Arpad Mike
Journal:  PLoS One       Date:  2010-12-20       Impact factor: 3.240

10.  Stereoselective effects of mexiletine enantiomers on sodium currents and excitability characteristics of adult skeletal muscle fibers.

Authors:  A De Luca; F Natuzzi; G Lentini; C Franchini; V Tortorella; D Conte Camerino
Journal:  Naunyn Schmiedebergs Arch Pharmacol       Date:  1995-12       Impact factor: 3.000
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