Abstract

The long term goal of this research is to understand the mechanisms of antiarrhythmic drug modification of the cardiac sodium channel. The experimental approach in this grant proposal combines the measurement of Na channel gating current, which are a direct measure of the channel's molecular conformational states, with modification of cardiac Na channels by toxins or agents to help understand antiarrhythmic drug interactions with the cardiac Na channel. In our present grant period we have found the applying this approach has made important advances in the understanding of antiarrhythmic drug modification of cardiac Na channels by QX-222 and lidocaine, and int he understanding of cardiac Na channel inactivation by the use of the site-3 toxin, Anthopleurin-A. For the next grant period we propose to continue our studies of cardiac Na inactivation, which has been shown to be important in the action of antiarrhythmic drugs, and of lidocaine's modification of cardiac Na channel gating currents. This grant proposal will use both native cardiac Na channels in single heart cell preparations and mutated cardiac Na channels expressed in large, fused tsA201 cells to study Na channels modified by lidocaine, by Na channel toxins and agents, and by site-directed mutagenesis.
The specific aims are; 1. Determine if batrachotoxin (BTX) modification of cardiac Na channels alters movement of the channels's voltage sensors similar to changes caused by the antiarrhythmic drug, lidocaine, and determine if either lidocaine or BTX inhibit movement of the voltage-sensor associated with cardiac Na channel inactivation from the open-state (OyieldsI inactivation). 2. Determine if the voltage-sensor associated with O yields I inactivation in cardiac Na channels is separate from the putative inactivation gate formed by the intracellular linker region between domains III and IV. 3. Determine if immobilization of off-gating charge in cardiac Na channels is associated with the putative inactivation gate. 4. Determine if the voltage-sensor for O yieldsI activation in cardiac Na channels is associated with the S4 segment of domain IV. 5. Determine if the cardiac Na channel gating charge-voltage relationship measured during step depolarizations to test potentials near INa threshold underestimates the total gating charge. The results of the proposed studies in the this grant should advance our understanding of the molecular mechanisms of cardiac Na channel inactivation, and our understanding of which components of the cardiac Na channel's voltage sensors are modified by lidocaine. In combination, they should contribute to the formation of a better molecular model of antiarrhythmic drug interactions with the cardiac Na channel, and form the foundation for future studies of antiarrhythmic drug-Na channel interactions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL044630-09
Application #
2857799
Study Section
Pharmacology A Study Section (PHRA)
Project Start
1990-04-01
Project End
2000-12-31
Budget Start
1999-01-01
Budget End
1999-12-31
Support Year
9
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Utah
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Sheets, Michael F; Fozzard, Harry A; Lipkind, Gregory M et al. (2010) Sodium channel molecular conformations and antiarrhythmic drug affinity. Trends Cardiovasc Med 20:16-21
Hanck, Dorothy A; Nikitina, Elena; McNulty, Megan M et al. (2009) Using lidocaine and benzocaine to link sodium channel molecular conformations to state-dependent antiarrhythmic drug affinity. Circ Res 105:492-9
Hanck, Dorothy A; Sheets, Michael F (2007) Site-3 toxins and cardiac sodium channels. Toxicon 49:181-93
Sheets, Michael F; Hanck, Dorothy A (2007) Outward stabilization of the S4 segments in domains III and IV enhances lidocaine block of sodium channels. J Physiol 582:317-34
Sheets, Michael F; Hanck, Dorothy A (2005) Charge immobilization of the voltage sensor in domain IV is independent of sodium current inactivation. J Physiol 563:83-93
Chen, Tiehua; Inoue, Masashi; Sheets, Michael F (2005) Reduced voltage dependence of inactivation in the SCN5A sodium channel mutation delF1617. Am J Physiol Heart Circ Physiol 288:H2666-76
Sheets, Michael F; Hanck, Dorothy A (2003) Molecular action of lidocaine on the voltage sensors of sodium channels. J Gen Physiol 121:163-75
Sheets, Michael F; Hanck, Dorothy A (2002) The outermost lysine in the S4 of domain III contributes little to the gating charge in sodium channels. Biophys J 82:3048-55
Hanck, D A; Makielski, J C; Sheets, M F (2000) Lidocaine alters activation gating of cardiac Na channels. Pflugers Arch 439:814-21
Sheets, M F; Kyle, J W; Hanck, D A (2000) The role of the putative inactivation lid in sodium channel gating current immobilization. J Gen Physiol 115:609-20

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