Abstract

Within the heart, exercise training increases coronary permeability- surface area product, an index of exchange capacity, by unknown mechanisms. The current view of the capillary exchange barrier has progressed from one of a static boundary to a dynamic structure involved in moment-to-moment regulation of gas, water, and solute movements between blood and tissue. Since surface area does not account for the observed training-induced increase of exchange capacity, this project focuses on microvessel permeability and applies the specialized techniques of this laboratory to measure microvessel transport. From these measurements the mechanisms responsible for coronary microvessel adaptation to exercise training will be elucidated. The primary hypothesis is that exercise training increases coronary microvessel permeability (Aims 1 & 2). Further, the studies are designed to determine whether training effects are local or systemic (Aim 3), whether exercise training alters the dynamic status of the vascular barrier (Aim 4), and/or whether changes in individual vessels contribute equally to the integrated responses of intact hearts (Aims 5). In resistance arteries and venules isolated from the heart and mesentery of sedentary ad exercise trained pigs, solute flux of fluorescent probes of known size and change, will be measured as a function of perfusion pressure. From these measurements the transport coefficients diffusive solute permeability (Pd) and solvent drag coefficient (Lp(1-sigma)) will be calculated. Permeability responses of the microvessels will be assessed under basal conditions and then following perfusion with endothelium- dependent and -independent vasodilators. Permeability/surface area product will also be measured, first, in whole hearts from sedentary and exercise trained pigs and, second, in resistance arteries and venules isolated from these same hearts. Knowledge of mechanisms that dictate control of permeability in individual microvessels and intact hearts will provide a basis for elucidating observed exercise training-induced increases in coronary exchange capacity. The key to understanding whether exercise training compensates for or reverses dysfunction caused by coronary disease also rests on a mechanistic approach to studying changes observed with training.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
1P01HL052490-01A1
Application #
3737291
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
1
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Missouri-Columbia
Department
Type
DUNS #
112205955
City
Columbia
State
MO
Country
United States
Zip Code
65211

  Publications

Masseau, I; Bowles, D K (2015) Carotid Endothelial VCAM-1 Is an Early Marker of Carotid Atherosclerosis and Predicts Coronary Artery Disease in Swine. J Biomed Sci Eng 8:789-796
Gole, Hope K A; Tharp, Darla L; Bowles, Douglas K (2014) Upregulation of intermediate-conductance Ca2+-activated K+ channels (KCNN4) in porcine coronary smooth muscle requires NADPH oxidase 5 (NOX5). PLoS One 9:e105337
McKenney, Mikaela L; Schultz, Kyle A; Boyd, Jack H et al. (2014) Epicardial adipose excision slows the progression of porcine coronary atherosclerosis. J Cardiothorac Surg 9:2
Heaps, Cristine L; Robles, Juan Carlos; Sarin, Vandana et al. (2014) Exercise training-induced adaptations in mediators of sustained endothelium-dependent coronary artery relaxation in a porcine model of ischemic heart disease. Microcirculation 21:388-400
Hamilton, Marc T; Hamilton, Deborah G; Zderic, Theodore W (2014) Sedentary behavior as a mediator of type 2 diabetes. Med Sport Sci 60:11-26
Bender, Shawn B; de Beer, Vincent J; Tharp, Darla L et al. (2014) Reduced contribution of endothelin to the regulation of systemic and pulmonary vascular tone in severe familial hypercholesterolaemia. J Physiol 592:1757-69
Simmons, Grant H; Padilla, Jaume; Jenkins, Nathan T et al. (2014) Exercise training and vascular cell phenotype in a swine model of familial hypercholesterolaemia: conduit arteries and veins. Exp Physiol 99:454-65
Fain, John N; Company, Joseph M; Booth, Frank W et al. (2013) Exercise training does not increase muscle FNDC5 protein or mRNA expression in pigs. Metabolism 62:1503-11
de Beer, Vincent J; Merkus, Daphne; Bender, Shawn B et al. (2013) Familial hypercholesterolemia impairs exercise-induced systemic vasodilation due to reduced NO bioavailability. J Appl Physiol (1985) 115:1767-76
Congdon, Kimberly A; Hammond, Ashley S; Ravosa, Matthew J (2012) Differential limb loading in miniature pigs (Sus scrofa domesticus): a test of chondral modeling theory. J Exp Biol 215:1472-83

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