Abstract

Adult mammalian myocardium adapts to chronic hemodynamic over loading by increasing the size of its constituent myocytes (hypertrophy). Previous studies have shown that functional electrophysiological and contractile alterations are associated with the (pressure-overload induced) hypertrophy process. The cellular basis for these changes have not been clearly defined to date because standard multicellular cardiac preparations are not well suited for experiments addressing these issues. Isolated single myocytes however (disaggregated from intact ventricular muscle with techniques developed recently) should serve as a useful model preparation for studies of this nature. In this regard, myocytes isolated from normal and hypertrophied feline right ventricles will serve as the experimental preparation in the present research. The long term objectives of this research is to elucidate changes in the excitation-contraction coupling process that might play a key role in the compensatory myocardial response to pressure and volume loading and/or the transition from compensated hypertrophy to heart failure. The hypothesis to be tested is that processes involved in Ca++ homeostasis are modified during hypertrophy and lead to the functional electrophysiological and contractile alterations of hypertrophied myocardium.
The specific aims of this research are 1. to determine if the Ca++ buffering capacity (and therefore free Ca++i) of hypertrophied feline myocytes is abnormal. 2. To determine if the electrophysiological and contractile alterations of hypertrophied myocytes are related to abnormalities in process involved in Ca++ homeostasis. 3. To determine if alterations in sarcolemmal Na/Ca exchange and/or sarcoplasmic reticular Ca++ release and/or uptake are specific factors leading to abnormal Ca++ handling by hypertrophied myocytes. To achieve these aims Ca++i and total cell Ca++ will be measured with Quin-2 and atomic absorbtion spectrophotometry respectively. Myocyte electrophysiological and contractile properties will be measured with microelectrode and photodiode techniques. The combined use of isolated myocytes and recetnly developed experimental techniques should provide significant new insight into the E-C coupling process in normal myocytes as well as the changes in this process that occur in hypertrophied myocardium.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL033921-03
Application #
3346302
Study Section
Cardiovascular Study Section (CVA)
Project Start
1985-06-01
Project End
1990-05-31
Budget Start
1987-06-01
Budget End
1988-05-31
Support Year
3
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

Name
Temple University
Department
Type
Schools of Medicine
DUNS #
City
Philadelphia
State
PA
Country
United States
Zip Code
19122

  Publications

Borghetti, Giulia; von Lewinski, Dirk; Eaton, Deborah M et al. (2018) Diabetic Cardiomyopathy: Current and Future Therapies. Beyond Glycemic Control. Front Physiol 9:1514
Wang, Wei Eric; Li, Liangpeng; Xia, Xuewei et al. (2017) Dedifferentiation, Proliferation, and Redifferentiation of Adult Mammalian Cardiomyocytes After Ischemic Injury. Circulation 136:834-848
Eschenhagen, Thomas; Bolli, Roberto; Braun, Thomas et al. (2017) Cardiomyocyte Regeneration: A Consensus Statement. Circulation 136:680-686
Sharp 3rd, Thomas E; Schena, Giana J; Hobby, Alexander R et al. (2017) Cortical Bone Stem Cell Therapy Preserves Cardiac Structure and Function After Myocardial Infarction. Circ Res 121:1263-1278
Cho, Gun-Sik; Lee, Dong I; Tampakakis, Emmanouil et al. (2017) Neonatal Transplantation Confers Maturation of PSC-Derived Cardiomyocytes Conducive to Modeling Cardiomyopathy. Cell Rep 18:571-582
Troupes, Constantine D; Wallner, Markus; Borghetti, Giulia et al. (2017) Role of STIM1 (Stromal Interaction Molecule 1) in Hypertrophy-Related Contractile Dysfunction. Circ Res 121:125-136
Wallner, Markus; Eaton, Deborah M; Berretta, Remus M et al. (2017) A Feline HFpEF Model with Pulmonary Hypertension and Compromised Pulmonary Function. Sci Rep 7:16587
Harper, Shavonn C; Brack, Andrew; MacDonnell, Scott et al. (2016) Is Growth Differentiation Factor 11 a Realistic Therapeutic for Aging-Dependent Muscle Defects? Circ Res 118:1143-50; discussion 1150
Wallner, Markus; Duran, Jason M; Mohsin, Sadia et al. (2016) Acute Catecholamine Exposure Causes Reversible Myocyte Injury Without Cardiac Regeneration. Circ Res 119:865-79
Leipsic, Jonathon A (2015) President's Page. J Cardiovasc Comput Tomogr 9:604-5

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