Literature DB >> 2409220

Interactions of monovalent cations with sodium channels in squid axon. I. Modification of physiological inactivation gating.

G S Oxford, J Z Yeh.   

Abstract

Inactivation of Na channels has been studied in voltage-clamped, internally perfused squid giant axons during changes in the ionic composition of the intracellular solution. Peak Na currents are reduced when tetramethylammonium ions (TMA+) are substituted for Cs ions internally. The reduction reflects a rapid, voltage-dependent block of a site in the channel by TMA+. The estimated fractional electrical distance for the site is 10% of the channel length from the internal surface. Na tail currents are slowed by TMA+ and exhibit kinetics similar to those seen during certain drug treatments. Steady state INa is simultaneously increased by TMA+, resulting in a "cross-over" of current traces with those in Cs+ and in greatly diminished inactivation at positive membrane potentials. Despite the effect on steady state inactivation, the time constants for entry into and exit from the inactivated state are not significantly different in TMA+ and Cs+. Increasing intracellular Na also reduces steady state inactivation in a dose-dependent manner. Ratios of steady state INa to peak INa vary from approximately 0.14 in Cs+- or K+-perfused axons to approximately 0.4 in TMA+- or Na+-perfused axons. These results are consistent with a scheme in which TMA+ or Na+ can interact with a binding site near the inner channel surface that may also be a binding or coordinating site for a natural inactivation particle. A simple competition between the ions and an inactivation particle is, however, not sufficient to account for the increase in steady state INa, and changes in the inactivation process itself must accompany the interaction of TMA+ and Na+ with the channel.

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Year:  1985        PMID: 2409220      PMCID: PMC2215803          DOI: 10.1085/jgp.85.4.583

Source DB:  PubMed          Journal:  J Gen Physiol        ISSN: 0022-1295            Impact factor:   4.086


  41 in total

1.  Kinetic and pharmacological properties of the sodium channel of frog skeletal muscle.

Authors:  D T Campbell; B Hille
Journal:  J Gen Physiol       Date:  1976-03       Impact factor: 4.086

2.  Negative surface charge near sodium channels of nerve: divalent ions, monovalent ions, and pH.

Authors:  B Hille; A M Woodhull; B I Shapiro
Journal:  Philos Trans R Soc Lond B Biol Sci       Date:  1975-06-10       Impact factor: 6.237

3.  The permeability of the sodium channel in Myxicola to the alkali cations.

Authors:  G A Ebert; L Goldman
Journal:  J Gen Physiol       Date:  1976-09       Impact factor: 4.086

4.  Rate constants associated with changes in sodium conductance in axons perfused with sodium fluoride.

Authors:  W K Chandler; H Meves
Journal:  J Physiol       Date:  1970-12       Impact factor: 5.182

5.  Evidence for two types of sodium conductance in axons perfused with sodium fluoride solution.

Authors:  W K Chandler; H Meves
Journal:  J Physiol       Date:  1970-12       Impact factor: 5.182

6.  Sodium and potassium currents in squid axons perfused with fluoride solutions.

Authors:  W K Chandler; H Meves
Journal:  J Physiol       Date:  1970-12       Impact factor: 5.182

7.  Ionic selectivity, saturation, and block in sodium channels. A four-barrier model.

Authors:  B Hille
Journal:  J Gen Physiol       Date:  1975-11       Impact factor: 4.086

8.  Ionic blockage of sodium channels in nerve.

Authors:  A M Woodhull
Journal:  J Gen Physiol       Date:  1973-06       Impact factor: 4.086

9.  Selective modification of sodium channel gating in lobster axons by 2, 4, 6-trinitrophenol: Evidence for two inactivation mechanisms.

Authors:  G S Oxford; J P Pooler
Journal:  J Gen Physiol       Date:  1975-12       Impact factor: 4.086

10.  Destruction of sodium conductance inactivation in squid axons perfused with pronase.

Authors:  C M Armstrong; F Bezanilla; E Rojas
Journal:  J Gen Physiol       Date:  1973-10       Impact factor: 4.086

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  26 in total

1.  Mechanisms of cation permeation in cardiac sodium channel: description by dynamic pore model.

Authors:  Y Kurata; R Sato; I Hisatome; S Imanishi
Journal:  Biophys J       Date:  1999-10       Impact factor: 4.033

2.  Steady-state availability of sodium channels. Interactions between activation and slow inactivation.

Authors:  P C Ruben; J G Starkus; M D Rayner
Journal:  Biophys J       Date:  1992-04       Impact factor: 4.033

3.  A sodium channel gating model based on single channel, macroscopic ionic, and gating currents in the squid giant axon.

Authors:  C A Vandenberg; F Bezanilla
Journal:  Biophys J       Date:  1991-12       Impact factor: 4.033

4.  Block of sodium channels by internal mono- and divalent guanidinium analogues. Modulation by sodium ion concentration.

Authors:  M Danko; C Smith-Maxwell; L McKinney; T Begenisich
Journal:  Biophys J       Date:  1986-02       Impact factor: 4.033

5.  Internal cesium and the sodium inactivation gate in Myxicola giant axons.

Authors:  L Goldman
Journal:  Biophys J       Date:  1986-08       Impact factor: 4.033

6.  Ion-channel entrances influence permeation. Net charge, size, shape, and binding considerations.

Authors:  J A Dani
Journal:  Biophys J       Date:  1986-03       Impact factor: 4.033

7.  Anomalous effect of permeant ion concentration on peak open probability of cardiac Na+ channels.

Authors:  C Townsend; H A Hartmann; R Horn
Journal:  J Gen Physiol       Date:  1997-07       Impact factor: 4.086

8.  Saxitoxin and tetrodotoxin. Electrostatic effects on sodium channel gating current in crayfish axons.

Authors:  S T Heggeness; J G Starkus
Journal:  Biophys J       Date:  1986-03       Impact factor: 4.033

9.  Gating kinetics of ATP-sensitive single potassium channels in myocardial cells depends on electromotive force.

Authors:  Y Zilberter; N Burnashev; A Papin; V Portnov; B Khodorov
Journal:  Pflugers Arch       Date:  1988-05       Impact factor: 3.657

10.  Reconstituted voltage-sensitive sodium channels from eel electroplax: activation of permeability by quaternary lidocaine, N-bromoacetamide, and N-bromosuccinimide.

Authors:  E C Cooper; W S Agnew
Journal:  J Membr Biol       Date:  1989-11       Impact factor: 1.843

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