Abstract

While prolongation of the action potential (AP) can be anti-arrhythmic, it is also the cause of many arrhythmias due to drugs, congenital disease, and heart failure. Much evidence implicates early after depolarizations (EADs) due to L-type Ca2+ current (ICa-L) as a trigger for arrhythmias associated with prolonged action potentials. We and others nave shown that multifunctional Ca2+/calmodulin - dependent protein kinase II (CaM kinase) augments ICa-L in response to increased intracellular Ca2+ ([Ca2+]i ), and increased [Ca 2+]i occurs during EADs and AP prolongation. Importantly, after initial activation, CaM kinase activity (unlike that of other kinases) becomes independent of [Ca2+]i. Therefore, the central hypothesis to be tested in this research is that CaM kinase acts as a [Ca2+]i dependent and a [Ca2+]i - independent positive feedback effector for ICa-L and thus serves as a key proarrhythmic signaling molecule for EADs. Moreover, our preliminary data also indicate CaM kinase is localized in myocytes to the Z-lines, raising the possibility that the action of CaM kinase on ICa-L and EADs is specified by an interaction among the kinase, specific anchoring proteins, and the cytoskeleton.
Four specific aims i n this research will determine (1) the role of [Ca2+]i and ICa-L in EADs in cardiac cells with prolonged action potentials; (2) the effect of CaM kinase inhibition on ICa-L, [Ca2+]i and EADs; (3) the effect of constitutively active CaM kinase on ICa-L, [Ca 2+]i, and EADs; and (4) the role the cytoskeleton and anchoring proteins in modulation of ICa-L, [Ca 2+]i, and EADs by CaM kinase. EADs will be studied in isolated rabbit ventricular myocytes with prolonged action potentials, using current clamp and whole cell mode voltage clamp with action potential wave forms, under conditions where [Ca2+]i is controlled and directly measured, ICa-L is directly measured, and CaM kinase activity is controlled with specific inhibitory peptides or the use of a constitutively active (Ca2+-independent) form of the enzyme. By furthering our understanding of the mechanisms underlying arrhythmias related to prolonged repolarization, this research should result in identification and initial validation of novel targets for suppression or these arrhythmias.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL062494-02
Application #
6184818
Study Section
Cardiovascular and Pulmonary Research A Study Section (CVA)
Project Start
1999-04-01
Project End
2003-03-31
Budget Start
2000-04-01
Budget End
2001-03-31
Support Year
2
Fiscal Year
2000
Total Cost
$146,900
Indirect Cost

  Institution

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

  Publications

Zhang, Caimei; Chen, Biyi; Guo, Ang et al. (2014) Microtubule-mediated defects in junctophilin-2 trafficking contribute to myocyte transverse-tubule remodeling and Ca2+ handling dysfunction in heart failure. Circulation 129:1742-50
Gao, Zhan; Rasmussen, Tyler P; Li, Yue et al. (2013) Genetic inhibition of Na+-Ca2+ exchanger current disables fight or flight sinoatrial node activity without affecting resting heart rate. Circ Res 112:309-17
Sierra, Ana; Zhu, Zhiyong; Sapay, Nicolas et al. (2013) Regulation of cardiac ATP-sensitive potassium channel surface expression by calcium/calmodulin-dependent protein kinase II. J Biol Chem 288:1568-81
Yang, Jianqi; Maity, Biswanath; Huang, Jie et al. (2013) G-protein inactivator RGS6 mediates myocardial cell apoptosis and cardiomyopathy caused by doxorubicin. Cancer Res 73:1662-7
DeGrande, Sean T; Little, Sean C; Nixon, Derek J et al. (2013) Molecular mechanisms underlying cardiac protein phosphatase 2A regulation in heart. J Biol Chem 288:1032-46
Chen, Biyi; Guo, Ang; Zhang, Caimei et al. (2013) Critical roles of junctophilin-2 in T-tubule and excitation-contraction coupling maturation during postnatal development. Cardiovasc Res 100:54-62
Klug, Jason R; Mathur, Brian N; Kash, Thomas L et al. (2012) Genetic inhibition of CaMKII in dorsal striatal medium spiny neurons reduces functional excitatory synapses and enhances intrinsic excitability. PLoS One 7:e45323
Gudmundsson, Hjalti; Curran, Jerry; Kashef, Farshid et al. (2012) Differential regulation of EHD3 in human and mammalian heart failure. J Mol Cell Cardiol 52:1183-90
Joiner, Mei-Ling A; Koval, Olha M; Li, Jingdong et al. (2012) CaMKII determines mitochondrial stress responses in heart. Nature 491:269-73
Chen, Biyi; Guo, Ang; Gao, Zhan et al. (2012) In situ confocal imaging in intact heart reveals stress-induced Ca(2+) release variability in a murine catecholaminergic polymorphic ventricular tachycardia model of type 2 ryanodine receptor(R4496C+/-) mutation. Circ Arrhythm Electrophysiol 5:841-9

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