Abstract

Patients with heart disease are frequently exposed to an abnormal and dynamic neurohormonal milieu, with resultant varying activation of cellular signalling systems. Available data indicate that most cardiac ion channels in native myocytes are regulated by cellular signalling systems. However, analysis of specific currents is complicated by the presence of multiple components most likely representing structurally distinct ion channels. This Project will combine electrophysiologic and biochemical methods to investigate the mechanisms by which cellular metabolic processes regulate the function of individual cardiac potassium channels. Cloned human and rat potassium channels expressed in a mammalian tissue culture system will be studied using whole-cell techniques to determine if stimulation of protein kinase A or C or alterations in intracellular calcium alter outward current; more detailed experiments using a range of modulators, including catalytic subunits of individual kinases, in excised and cell-attached patches will determine the electrophysiologic mechanisms of such modulation. Parallel studies will be conducted in native myocytes displaying outward current resembling that of the clones. Bacterially synthesized fusion proteins will be used to directly determine the extent to which cloned channel proteins can serve as substrates for phosphorylation by protein kinase A and C, and specific phosphorylated residues will be mapped using HPLC and mass spectrometry. Amino acids identified as phosphorylation sites will be mutated and the functional consequences for the electrophysiology and response to cellular regulation of the mutant protein determined. The effects of ion channel blockers on metabolically stimulated and unstimulated channels will be compared to determine if response to blockers and to stimulation is additive, or if response to blockers is qualitatively altered in stimulated systems. These studies will determine mechanisms and functional consequences of ion channel phosphorylation and may thereby identify circumstances in which arrhythmia provocation or altered antiarrhythmic drug effect occur in patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
1P01HL046681-01A1
Application #
3844966
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Yang, Tao; Smith, Jarrod A; Leake, Brenda F et al. (2013) An allosteric mechanism for drug block of the human cardiac potassium channel KCNQ1. Mol Pharmacol 83:481-9
Hayashi, Kenshi; Shuai, Wen; Sakamoto, Yuichiro et al. (2010) Trafficking-competent KCNQ1 variably influences the function of HERG long QT alleles. Heart Rhythm 7:973-80
Yang, Tao; McBride, Brian F; Leake, Brenda F et al. (2010) Modulation of drug block of the cardiac potassium channel KCNA5 by the drug transporters OCTN1 and MDR1. Br J Pharmacol 161:1023-33
Stepanovic, Svetlana Z; Potet, Franck; Petersen, Christina I et al. (2009) The evolutionarily conserved residue A653 plays a key role in HERG channel closing. J Physiol 587:2555-66
Yang, Tao; Chung, Seo-Kyung; Zhang, Wei et al. (2009) Biophysical properties of 9 KCNQ1 mutations associated with long-QT syndrome. Circ Arrhythm Electrophysiol 2:417-26
Potet, Franck; Petersen, Christina I; Boutaud, Olivier et al. (2009) Genetic screening in C. elegans identifies rho-GTPase activating protein 6 as novel HERG regulator. J Mol Cell Cardiol 46:257-67
Yang, Tao; Kanki, Hideaki; Zhang, Wei et al. (2009) Probing the mechanisms underlying modulation of quinidine sensitivity to cardiac I(Ks) block by protein kinase A-mediated I(Ks) phosphorylation. Br J Pharmacol 157:952-61
Grueter, Chad E; Abiria, Sunday A; Wu, Yunji et al. (2008) Differential regulated interactions of calcium/calmodulin-dependent protein kinase II with isoforms of voltage-gated calcium channel beta subunits. Biochemistry 47:1760-7
Baudenbacher, Franz; Schober, Tilmann; Pinto, Jose Renato et al. (2008) Myofilament Ca2+ sensitization causes susceptibility to cardiac arrhythmia in mice. J Clin Invest 118:3893-903
Makita, Naomasa; Behr, Elijah; Shimizu, Wataru et al. (2008) The E1784K mutation in SCN5A is associated with mixed clinical phenotype of type 3 long QT syndrome. J Clin Invest 118:2219-29

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