Abstract

Normal heart function is dependent on the Frank-Starling mechanism of matching stroke volume to venous return to adjust cardiac output with changes in metabolic demand. This mechanism is often diminished in cardiac disease. Our studies have lead us to believe that the steep sarcomere length-dependence of Ca2+ activated force in cardiac muscle (the cellular basis of the Frank-Starling mechanism) results from the properties of cardiac thin filaments and interaction with myosin cross-bridges. These are determined by 1) the isoform specific properties of thin filament regulatory proteins, 2) the unique dependence of Ca2+ binding to cardiac thin filaments in force generation and 3) the effects of length-dependent changes in cross-bridge proximity in thin filament activation. Physiologically, cardiac force sensitivity to [Ca2+] is regulated by altered phosphorylation of contractile proteins, including TF regulatory subunits, myosin regulatory light chains, myosin-binding protein-C and titin. The protein phosphorylation profile of the heart changes during cardiac disease. It was recently demonstrated that depressed force generating capacity in failing hearts was enhanced by interventions that selectively increased cross-bridge access to cardiac thin filaments by stimulating phosphorylation of selected cardiac proteins. In this study we will determine the effect that phosphorylation of specific proteins has on cardiac contractility, in isolation from other potential sites of phosphorylation. We will also determine how phosphorylation effects are altered by FHC mutations of cTnI and how they influence stretch activation of cardiac muscle. Better understanding the molecular mechanism of the sarcomere length dependence of contraction should lead to targeted therapeutics to treat heart disease and failure. Force generation by the heart is modified by adding or removing phosphate groups from contractile proteins during both normal and diseased physiological states. Detailed knowledge of the interactions between the molecular components of the heart's contractile mechanism to be obtained in this study are key to designing ways to compensate for heart failure following an ischemic heart attack, prolonged cardiac failure or genetic disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
2R01HL067071-05A2
Application #
7464852
Study Section
Special Emphasis Panel (ZRG1-CVS-P (03))
Program Officer
Przywara, Dennis
Project Start
2001-05-10
Project End
2011-06-30
Budget Start
2009-07-01
Budget End
2010-06-30
Support Year
5
Fiscal Year
2009
Total Cost
$390,000
Indirect Cost

  Institution

Name
University of Washington
Department
Engineering (All Types)
Type
Schools of Medicine
DUNS #
605799469
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Leo, M Dennis; Bannister, John P; Narayanan, Damodaran et al. (2014) Dynamic regulation of ?1 subunit trafficking controls vascular contractility. Proc Natl Acad Sci U S A 111:2361-6
Rao, Vijay S; Korte, F Steven; Razumova, Maria V et al. (2013) N-terminal phosphorylation of cardiac troponin-I reduces length-dependent calcium sensitivity of contraction in cardiac muscle. J Physiol 591:475-90
Martyn, D A; Smith, L; Kreutziger, K L et al. (2007) The effects of force inhibition by sodium vanadate on cross-bridge binding, force redevelopment, and Ca2+ activation in cardiac muscle. Biophys J 92:4379-90
Xu, Sengen; Martyn, Donald; Zaman, Jessica et al. (2006) X-ray diffraction studies of the thick filament in permeabilized myocardium from rabbit. Biophys J 91:3768-75
Clemmens, Emilie Warner; Entezari, Michelle; Martyn, Donald A et al. (2005) Different effects of cardiac versus skeletal muscle regulatory proteins on in vitro measures of actin filament speed and force. J Physiol 566:737-46
Regnier, M; Martin, H; Barsotti, R J et al. (2004) Cross-bridge versus thin filament contributions to the level and rate of force development in cardiac muscle. Biophys J 87:1815-24
Adhikari, Bishow B; Regnier, Michael; Rivera, Anthony J et al. (2004) Cardiac length dependence of force and force redevelopment kinetics with altered cross-bridge cycling. Biophys J 87:1784-94
Martyn, Donald A; Adhikari, Bishow B; Regnier, Michael et al. (2004) Response of equatorial x-ray reflections and stiffness to altered sarcomere length and myofilament lattice spacing in relaxed skinned cardiac muscle. Biophys J 86:1002-11
Bin, Liang-Hua; Nielson, Larry D; Liu, Xinqi et al. (2003) Identification of uteroglobin-related protein 1 and macrophage scavenger receptor with collagenous structure as a lung-specific ligand-receptor pair. J Immunol 171:924-30