Abstract

. The broad, long-term objectives of the proposed research are to elucidate mechanisms underlying the regulation of myocardial contraction by diacylglycerol and protein kinase C. Many extracellular chemical signals such as hormones, neurotransmitters, cytokines, growth factors, mechanical stress and oxygen stress may regulate cardiac contractility by mobilizing lipid second messengers including diacylglycerol and cis- unsaturated fatty acids. There are at least four enzyme systems, PLA2, PLC-beta, PLC-gamma and PLD involved in generating these lipid messengers giving rise to a potentially information-rich signal encoded in lipid species generating these lipid messengers giving rise to a potentially information-rich signal encoded in lipid species, timing and location in a systematic way in order to establish the influence of these parameters on contractile regulation. cis-Unsaturated fatty acids and Ca will be investigated as putative co-messengers with diacylglycerol that may selectively activate protein kinase C isoforms alpha, epsilon or delta. The mechanisms of protein kinase C anchoring to sites on the transverse tubules and to sites on the myofilament will be examined and their respective roles in regulating systolic Ca levels and myofilament Ca sensitivity will be established. Whether protein kinase C mediated phosphorylation of cardiac troponin I is a major mechanism underlying positive or negative inotropic responses in ventricular myocytes will also be established. The goal is to use a combination of modern and innovative methodologies in cell biophysics, imaging and molecular biology to provide unambiguous answers to fundamental questions about diacylglycerol signaling in the heart. This research will further our understanding of basic mechanisms by which lipid messengers alter cardiac physiology, and mechanisms of protein kinase C regulation of cardiac troponin I function, so that defects in these pathways in various diseased states can be identified and corrected. The proposed research will be highly interactive with other subprojects and will rely to a significant extent on the expertise of other investigators in the Program. Overall, this research addresses a major theme of the Program involving elucidation of signal transduction mechanisms evoked by membrane receptor antagonists in myocardium.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
3P01HL047053-08S1
Application #
6643674
Study Section
Project Start
2002-06-01
Project End
2003-05-31
Budget Start
Budget End
Support Year
8
Fiscal Year
2002
Total Cost
$199,591
Indirect Cost

  Institution

Name
University of Wisconsin Madison
Department
Type
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715

  Publications

Druckenbrod, Noah R; Powers, Patricia A; Bartley, Christopher R et al. (2008) Targeting of endothelin receptor-B to the neural crest. Genesis 46:396-400
Brickson, S; Fitzsimons, D P; Pereira, L et al. (2007) In vivo left ventricular functional capacity is compromised in cMyBP-C null mice. Am J Physiol Heart Circ Physiol 292:H1747-54
Vatta, Matteo; Ackerman, Michael J; Ye, Bin et al. (2006) Mutant caveolin-3 induces persistent late sodium current and is associated with long-QT syndrome. Circulation 114:2104-12
Stelzer, Julian E; Larsson, Lars; Fitzsimons, Daniel P et al. (2006) Activation dependence of stretch activation in mouse skinned myocardium: implications for ventricular function. J Gen Physiol 127:95-107
Stelzer, Julian E; Fitzsimons, Daniel P; Moss, Richard L (2006) Ablation of myosin-binding protein-C accelerates force development in mouse myocardium. Biophys J 90:4119-27
Singla, Dinender K; Hacker, Timothy A; Ma, Lining et al. (2006) Transplantation of embryonic stem cells into the infarcted mouse heart: formation of multiple cell types. J Mol Cell Cardiol 40:195-200
Muthukumarana, Poorni A D S; Lyons, Gary E; Miura, Yuji et al. (2006) Evidence for functional inter-relationships between FOXP3, leukaemia inhibitory factor, and axotrophin/MARCH-7 in transplantation tolerance. Int Immunopharmacol 6:1993-2001
Stelzer, Julian E; Patel, Jitandrakumar R; Moss, Richard L (2006) Acceleration of stretch activation in murine myocardium due to phosphorylation of myosin regulatory light chain. J Gen Physiol 128:261-72
Stelzer, Julian E; Patel, Jitandrakumar R; Moss, Richard L (2006) Protein kinase A-mediated acceleration of the stretch activation response in murine skinned myocardium is eliminated by ablation of cMyBP-C. Circ Res 99:884-90
Balijepalli, Ravi C; Foell, Jason D; Hall, Duane D et al. (2006) Localization of cardiac L-type Ca(2+) channels to a caveolar macromolecular signaling complex is required for beta(2)-adrenergic regulation. Proc Natl Acad Sci U S A 103:7500-5

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