Literature DB >> 17051346

Membrane potentials in Rana temporaria muscle fibres in strongly hypertonic solutions.

James A Fraser1, Kai Yuen Wong, Juliet A Usher-Smith, Christopher L-H Huang.   

Abstract

Conventional microelectrode methods were used to measure variations in resting membrane potentials, E(m), of intact amphibian skeletal muscle fibres over a wide range of increased extracellular tonicities produced by inclusion of varying extracellular concentrations of sucrose. Moderate increases in extracellular tonicity to up to 2.6x normal (2.6tau) under Cl(-) free conditions produced negative shifts in E(m) that followed expectations for the K(+) Nernst equation (E(K)) applied to a perfect osmometer containing a conserved intracellular K(+) content despite any accompanying cell volume change. In contrast, E(m) remained stable in fibres studied in otherwise similar Cl(-) containing solutions, consistent with E(m) stabilization despite negative shifts in E(K) through inward cation-Cl(-) co-transport activity. Short exposures to higher tonicities (>3tau) similarly produced negative shifts in E(m) in Cl(-) free but not Cl(-) containing solutions. However, prolonged exposures to solutions of >3tau caused gradual net positive changes in E (m) in both Cl(-) containing and Cl(-) free solutions suggesting that these changes were independent of cation-Cl(-) transport. Indeed, there was no evidence of cation-Cl(-) co-transport activity in strongly hypertonic solutions despite its predicted energetic favourability, suggesting its possible regulation by E (m) in muscle. Additional findings implicated a failure to maintain greatly increased transmembrane [K(+)] gradients in these E(m) changes. Thus: (1) halving or doubling [K(+)](e) produced negative or positive shifts in E(m), respectively in isotonic or moderately hypertonic (<2.7tau), but not strongly hypertonic (>3tau) solutions; (2) subsequent restoration of isotonic extracellular conditions produced further positive changes in E(m) consistent with a dilution of the depleted [K(+)](i) by fibres regaining their original resting volumes; (3) quantitative modelling similarly predicted a gradual net efflux of K(+) as the balance between active and passive [K(+)] fluxes altered due to increased transmembrane [K(+)] gradients in hypertonic and low [K(+)](e) solutions. However, the observed positive changes in E(m) in the most strongly hypertonic solutions eventually exceeded these predictions suggesting additional limitations on Na(+)/K(+)-ATPase activity in strongly hypertonic solutions.

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Year:  2006        PMID: 17051346     DOI: 10.1007/s10974-006-9091-4

Source DB:  PubMed          Journal:  J Muscle Res Cell Motil        ISSN: 0142-4319            Impact factor:   2.698


  24 in total

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Authors:  Emily A Ferenczi; James A Fraser; Sangeeta Chawla; Jeremy N Skepper; Christof J Schwiening; Christopher L-H Huang
Journal:  J Physiol       Date:  2003-12-23       Impact factor: 5.182

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  3 in total

1.  Conduction velocities in amphibian skeletal muscle fibres exposed to hyperosmotic extracellular solutions.

Authors:  Zhongbo Chen; Sandeep S Hothi; Wei Xu; Christopher L-H Huang
Journal:  J Muscle Res Cell Motil       Date:  2007-09-22       Impact factor: 2.698

2.  The determinants of transverse tubular volume in resting skeletal muscle.

Authors:  Jingwei Sim; James A Fraser
Journal:  J Physiol       Date:  2014-11-10       Impact factor: 5.182

3.  Inhibitory control over Ca(2+) sparks via mechanosensitive channels is disrupted in dystrophin deficient muscle but restored by mini-dystrophin expression.

Authors:  Martin D H Teichmann; Frederic V Wegner; Rainer H A Fink; Jeffrey S Chamberlain; Bradley S Launikonis; Boris Martinac; Oliver Friedrich
Journal:  PLoS One       Date:  2008-11-04       Impact factor: 3.240

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