Literature DB >> 9876137

State-dependent cocaine block of sodium channel isoforms, chimeras, and channels coexpressed with the beta1 subunit.

S N Wright1, S Y Wang, Y F Xiao, G K Wang.   

Abstract

Cocaine block of human cardiac (hH1) and rat skeletal (mu1) muscle sodium channels was examined under whole-cell voltage clamp in transiently transfected HEK293t cells. Low affinity block of resting mu1 and hH1 channels at -180 mV was the same, and high affinity block of inactivated channels at -70 mV was the same. Cocaine block of hH1 channels was greater than block of mu1 channels at voltages between -120 mV and -90 mV, suggesting that greater steady-state inactivation of hH1 channels in this voltage range makes them more susceptible to cocaine block. We induced shifts in the voltage dependence of steady-state inactivation at mu1 and hH1 channels by constructing mu1/hH1 channel chimeras or by coexpressing the wild-type channels with the rat brain beta1 subunit. In contrast to several previous reports, coexpression of the rat brain beta1 subunit with mu1 or hH1 produced large positive shifts in steady-state inactivation. Shifts in the voltage dependence of steady-state inactivation elicited linear shifts in steady-state cocaine block, yet these manipulations did not affect the cocaine affinity of resting or inactivated channels. These data, as well as simulations used to predict block, indicate that state-dependent cocaine block depends on both steady-state inactivation and channel activation, although inactivation appears to have the predominant role.

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Year:  1999        PMID: 9876137      PMCID: PMC1302514          DOI: 10.1016/S0006-3495(99)77192-4

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


  35 in total

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3.  Comparison of heterologously expressed human cardiac and skeletal muscle sodium channels.

Authors:  D W Wang; A L George; P B Bennett
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4.  A mutation in segment I-S6 alters slow inactivation of sodium channels.

Authors:  S Y Wang; G K Wang
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5.  Differences in the binding sites of two site-3 sodium channel toxins.

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6.  Primary structure and functional expression of a mammalian skeletal muscle sodium channel.

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7.  Independent versus coupled inactivation in sodium channels. Role of the domain 2 S4 segment.

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8.  Improved patch-clamp techniques for high-resolution current recording from cells and cell-free membrane patches.

Authors:  O P Hamill; A Marty; E Neher; B Sakmann; F J Sigworth
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9.  Characterization of cocaine-induced block of cardiac sodium channels.

Authors:  W J Crumb; C W Clarkson
Journal:  Biophys J       Date:  1990-03       Impact factor: 4.033

10.  Lidocaine block of cardiac sodium channels.

Authors:  B P Bean; C J Cohen; R W Tsien
Journal:  J Gen Physiol       Date:  1983-05       Impact factor: 4.086

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  14 in total

1.  Isoform-specific lidocaine block of sodium channels explained by differences in gating.

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

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3.  Block of persistent late Na+ currents by antidepressant sertraline and paroxetine.

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4.  Comparison of slow inactivation in human heart and rat skeletal muscle Na+ channel chimaeras.

Authors:  J P O'Reilly; S Y Wang; R G Kallen; G K Wang
Journal:  J Physiol       Date:  1999-02-15       Impact factor: 5.182

5.  Comparison of aconitine-modified human heart (hH1) and rat skeletal (mu1) muscle Na+ channels: an important role for external Na+ ions.

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Journal:  J Physiol       Date:  2002-02-01       Impact factor: 5.182

6.  Single point mutations affect fatty acid block of human myocardial sodium channel alpha subunit Na+ channels.

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Review 7.  Role of voltage-gated sodium, potassium and calcium channels in the development of cocaine-associated cardiac arrhythmias.

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8.  Study of procaine and tetracaine in the lipid bilayer using molecular dynamics simulation.

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9.  Comparative effects of halogenated inhaled anesthetics on voltage-gated Na+ channel function.

Authors:  Wei Ouyang; Karl F Herold; Hugh C Hemmings
Journal:  Anesthesiology       Date:  2009-03       Impact factor: 7.892

10.  Voltage-dependent inhibition of rat skeletal muscle sodium channels by aminoglycoside antibiotics.

Authors:  Adrian J Yeiser; James R Cox; Sterling N Wright
Journal:  Pflugers Arch       Date:  2004-02-13       Impact factor: 3.657

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