Abstract

The long term objectives of this proposal are (1) to understand the genetic regulation sarcoplasmic reticulum (SR) Ca2+ ATPase ene expression and 2 to define the role of altered SR Ca2+ ATPase expression in normal cardiac performance and congestive heart failure. The SR Ca2+ ATPase plays a central role in excitation contraction coupling of cardiac muscle. It is primarily responsible for the active transport of calcium into the SR vesicle. This lowers cytosolic calcium levels, thus permitting muscle relaxation. Recent findings suggest that the SR Ca2+ ATPase mRNA/protein levels and Ca2+ uptake function are substantially reduced in a coordinate fashion both in animal models of cardiac hypertrophy and in end stage human heart failure. Despite the obvious importance of SR Ca2+ ATPase in cardiac muscle physiology and possibly pathophysiology, relatively little is known of the mechanisms that regulate its' expression. There is data to suggest that SR Ca2+ ATPase is controlled at the level of transcription. Therefore, a primary goal of this proposal is to dissect the cis and trans-regulatory mechanisms controlling SR Ca2+ ATPase gene expression during normal and pathological states of the heart, as we hypothesize that the myocardial dysfunction in congestive heart failure is a partial consequence of altered Ca2+ ATPase expression. A second major goal of this proposal is to test this hypothesis directly in the whole animal by perturbing SR Ca2+ ATPase expression levels. To achieve these objectives, the following specific aims will be pursued: 1) Delineate cis-DNA control elements involved in transcriptional regulation of the SR Ca2+ ATPase gene in cardiac and skeletal muscle cells; 2) Identify nuclear protein factors that interact specifically with the SERCA2 promoter and modulate gene expression; 3) Delineate cis-DNA control elements responsible for tissue specific and pathophysiological regulation of the SR Ca2+ ATPase gene under in vivo conditions; 4) Create a transgenic animal model with alterations in SR Ca2+ transport function; and 5) Determine alterations in SR Ca2+ transport protein expression in early and late human congestive heart failure, and to relate these changes to hemodynamic indices of cardiac function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Specialized Center (P50)
Project #
5P50HL052318-02
Application #
5214180
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Shaikh, Sana A; Sahoo, Sanjaya K; Periasamy, Muthu (2016) Phospholamban and sarcolipin: Are they functionally redundant or distinct regulators of the Sarco(Endo)Plasmic Reticulum Calcium ATPase? J Mol Cell Cardiol 91:81-91
Kwong, Jennifer Q; Molkentin, Jeffery D (2015) Physiological and pathological roles of the mitochondrial permeability transition pore in the heart. Cell Metab 21:206-214
Karch, Jason; Molkentin, Jeffery D (2015) Regulated necrotic cell death: the passive aggressive side of Bax and Bak. Circ Res 116:1800-9
Liu, Ruijie; Correll, Robert N; Davis, Jennifer et al. (2015) Cardiac-specific deletion of protein phosphatase 1? promotes increased myofilament protein phosphorylation and contractile alterations. J Mol Cell Cardiol 87:204-13
Correll, Robert N; Eder, Petra; Burr, Adam R et al. (2014) Overexpression of the Na+/K+ ATPase ?2 but not ?1 isoform attenuates pathological cardiac hypertrophy and remodeling. Circ Res 114:249-256
van Berlo, Jop H; Kanisicak, Onur; Maillet, Marjorie et al. (2014) c-kit+ cells minimally contribute cardiomyocytes to the heart. Nature 509:337-41
Maurya, Santosh K; Periasamy, Muthu; Bal, Naresh C (2013) High gender -specific susceptibility to curare- a neuromuscular blocking agent. Biol Res 46:75-8
Molkentin, Jeffery D (2013) Parsing good versus bad signaling pathways in the heart: role of calcineurin-nuclear factor of activated T-cells. Circ Res 113:16-9
Davis, Jennifer; Maillet, Marjorie; Miano, Joseph M et al. (2012) Lost in transgenesis: a user's guide for genetically manipulating the mouse in cardiac research. Circ Res 111:761-77
Wu, Xu; Eder, Petra; Chang, Baojun et al. (2010) TRPC channels are necessary mediators of pathologic cardiac hypertrophy. Proc Natl Acad Sci U S A 107:7000-5

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