CAPSAICIN REGULATES VOLTAGE-DEPENDENT SODIUM CHANNELS BY ALTERING LIPID BILAYER ELASTICITY

doi:10.1124/mol.105.013573

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First published on June 20, 2005; DOI: 10.1124/mol.105.013573

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Received for publication April 22, 2005.
Revised June 17, 2005.
Accepted for publication June 20, 2005.

CAPSAICIN REGULATES VOLTAGE-DEPENDENT SODIUM CHANNELS BY ALTERING LIPID BILAYER ELASTICITY

Jens Lundbaek ¹^*, P. Birn ², S. E. Tape ³, Gill E. S. Toombes ⁴, Rikke S. R. Sogaard ⁵, Roger E. Koeppe II ⁶, Sol M. Gruner ⁴, Anker J. Hansen ², Olaf S. Andersen ⁷

¹ Weill Medical College of Cornell University ² Novo Nordisk A/S ³ Cornell University, Weill Medical College ⁴ Department of Physics, Cornell University ⁵ Institute of Biological Psychiatry, St. Hans Hospital, Denmark ⁶ Department of Chemistry and Biochemistry, University of Arkansas ⁷ Department of Physiology and Biophysics, Cornell University, Weill Medical College

^* Address correspondence to: E-mail: lundbaek{at}dadlnet.dk

Abstract

At sub-micromolar concentrations, capsaicin activates specificallythe TRPV1 receptor involved in nociception. At micro- to millimolarconcentrations, commonly used in clinical and in vitro studies,capsaicin also modulates the function of a large number of seeminglyunrelated membrane proteins, many of which are similarly modulatedby the capsaicin antagonist capsazepine. The mechanism(s) underlyingthis wide-spread regulation of protein function are not understood. We investigated whether capsaicin could regulate membrane proteinfunction by changing the elasticity of the host lipid bilayer. This was done by studying capsaicin's effects on lipid bilayerstiffness, measured using gramicidin A (gA) channels as molecularforce-transducers, and on voltage-dependent sodium channels(VDSC) known to be regulated by bilayer elasticity. Capsaicinand capsazepine (10 - 100 µM) increase gA channel appearancerate and lifetime without measurably altering bilayer thicknessor channel conductance, meaning that the changes in bilayerelasticity are sufficient to alter the conformation of an embeddedprotein. Capsaicin and capsazepine promote VDSC inactivation,similar to other amphiphiles that decrease bilayer stiffness,producing use-dependent current inhibition. For capsaicin thequantitative relation between the decrease in bilayer stiffnessand the hyperpolarizing shift in inactivation conforms to thatpreviously found for other amphiphiles. Capsaicin's effectson gA channels and VDSC are similar to those of Triton X-100,though these amphiphiles promote opposite lipid monolayer curvature. We conclude that capsaicin can regulate VDSC function by alteringbilayer elasticity. This mechanism may underlie the promiscuousregulation of membrane protein function by capsaicin and capsazepine- and by amphiphilic drugs generally.

Key words: Ion channel regulation, Sodium

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