Abstract

Experimental and clinical approaches for treating heart failure (HF) have traditionally focused on interrupting processes involved with its development, and in particular, understanding and preventing the transition from adaptive to maladaptive left ventricular hypertrophy (LVH). This application argues for an alternative paradigm that focuses on myocardial recovery rather than injury. In models of pressure-relief and pharmacologic LVH regression in mice, we have demonstrated that myocardial recovery, including from failing hearts, is associated with structural and genomic patterns that are distinct from factors associated with LVH development. Mechanistically, although nuclear factor kappa B (NF-:B) is known to be involved in promoting LVH, we have shown that this transcription factor can independently regulate many recovery genes and processes, including the balance of survival and apoptotic signals. Our global hypothesis is that myocardial recovery can be independently studied and targeted for therapy. The objective of this application is to define when and how the heart can recover from a decompensated state. We will use NF-:B as a molecular tool to characterize mechanisms necessary for reverse remodeling. We will achieve our objective by pursuing the following aims: (1) Characterize the cellular and genomic response following relief of pressure overload by expanding our existing model to create a detailed pathologic and genomic framework for reverse remodeling of both the compensated and decompensated heart, including determining when recovery is no longer feasible. (2) Determine the effect of NF-:B inactivation on myocardial recovery by generating and functionally testing the effect of pressure-relief on conditional, cardiac-specific NF-:B knockout mice. (3) Determine the mechanistic role of NF-:B in myocardial recovery by evaluating the functional phase-dependent influence of NF-:B to promote survival or death pathways following pressure relief. This proposal is innovative in that it focuses on the recovery arm of LVH and HF. We expect to generate a molecular program of myocardial mass regression that will significantly contribute to the overall understanding of hypertrophy and heart failure. We envision a novel therapeutic paradigm that targets the system of myocardial repair as well as injury. Ultimately, these results will have a relevant and positive impact on treatment algorithms for the large number of HF patients.

Public Health Relevance

Heart failure is a growing epidemic in our society that contributes to significant morbidity and mortality. Whereas most current therapies are aimed at preventing or halting progression of detrimental heart remodeling, we propose an alternative approach that would try to reverse existing disease. We envision an innovative treatment paradigm that would link preventive and regressive therapy to favorably impact outcomes in this devastating disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL089592-04
Application #
8319345
Study Section
Cardiac Contractility, Hypertrophy, and Failure Study Section (CCHF)
Program Officer
Schwartz, Lisa
Project Start
2009-09-01
Project End
2014-06-30
Budget Start
2012-07-01
Budget End
2013-06-30
Support Year
4
Fiscal Year
2012
Total Cost
$372,488
Indirect Cost
$124,988

  Institution

Name
University of Utah
Department
Surgery
Type
Schools of Medicine
DUNS #
009095365
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Bowen, Megan E; Liu, Xiaoqing; Sundwall, Peter M et al. (2018) Right ventricular involution: What can we learn from nature's model of compensated hypertrophy? J Thorac Cardiovasc Surg 155:2024-2028.e1
Healy, Aaron H; McKellar, Stephen H; Drakos, Stavros G et al. (2016) Physiologic effects of continuous-flow left ventricular assist devices. J Surg Res 202:363-71
Koliopoulou, Antigone; McKellar, Stephen H; Rondina, Matthew et al. (2016) Bleeding and thrombosis in chronic ventricular assist device therapy: focus on platelets. Curr Opin Cardiol 31:299-307
Healy, Aaron H; Stehlik, Josef; Edwards, Leah B et al. (2016) Predictors of 30-day post-transplant mortality in patients bridged to transplantation with continuous-flow left ventricular assist devices--An analysis of the International Society for Heart and Lung Transplantation Transplant Registry. J Heart Lung Transplant 35:34-9
Diakos, Nikolaos A; Navankasattusas, Sutip; Abel, E Dale et al. (2016) Evidence of Glycolysis Up-Regulation and Pyruvate Mitochondrial Oxidation Mismatch During Mechanical Unloading of the Failing Human Heart: Implications for Cardiac Reloading and Conditioning. JACC Basic Transl Sci 1:432-444
Witman, Melissa A H; Garten, Ryan S; Gifford, Jayson R et al. (2015) Further Peripheral Vascular Dysfunction in Heart Failure Patients With a Continuous-Flow Left Ventricular Assist Device: The Role of Pulsatility. JACC Heart Fail 3:703-11
Selzman, Craig H; Madden, Jesse L; Healy, Aaron H et al. (2015) Bridge to removal: a paradigm shift for left ventricular assist device therapy. Ann Thorac Surg 99:360-7
Javan, Hadi; Szucsik, Amanda M; Li, Ling et al. (2015) Cardiomyocyte p65 nuclear factor-?B is necessary for compensatory adaptation to pressure overload. Circ Heart Fail 8:109-18
McKellar, Stephen H; Javan, Hadi; Bowen, Megan E et al. (2015) Animal model of reversible, right ventricular failure. J Surg Res 194:327-33
Madden, Jesse L; Drakos, Stavros G; Stehlik, Josef et al. (2014) Baseline red blood cell osmotic fragility does not predict the degree of post-LVAD hemolysis. ASAIO J 60:524-8

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