Abstract

The long-term goal of this proposal is to define the mechanism responsible for the reduced maximal exercise capacity of patients with heart failure. Prior observations suggest that this exercise intolerance is caused by underperfusion of skeletal muscle with resultant early muscle glycolysis and that the muscle underperfusion is due at least in part to impaired muscle arteriolar dilation. This proposal's specific objectives are 1) to clarify the prevalence of and mechanisms for impaired muscle arteriolar vasodilation in heart failure, 2) to determine if early muscle glycolysis in heart failure is due to a reduction in muscle O2 delivery and/or muscle oxidative capacity, and 3) to determine if muscle fatigue is due to muscle lactic acidosis. Muscle arteriolar behavior during exercise will be compared in patients with heart failure and normal subjects during forearm exercise and maximal bicycle exercise. Plethysmography will be used to measure forearm flow. A femoral venous thermodilution catheter will be used to measure leg flow. Muscle arteriolar behavior will be further characterized by examining maximal forearm vasodilatory capacity, forearm vascular responsiveness to intraarterial norepinephrine and angiotensin II, and forearm vascular responses to diuresis, digitalis and chronic angiotensin-converting enzyme inhibition. To clarify the relation of muscle metabolism to O2 delivery and muscle oxidative capacity, forearm flow will be correlated with forearm metabolism, measured with 31P NMR. The effect of increasing muscle O2 delivery on exercising forearm and leg muscles will be examined. Skeletal muscle biopsies will be analyzed for enzyme activities, capillarity and fiber type. To determine if lactate limits exercise, the effect of reducing muscle lactate accumulation with dichloroacetate will be examined. Parallel dog studies will be performed in a canine model of heart failure produced by chronic rapid ventricular pacing. Skeletal muscle arteriolar behavior will be assessed in the femoral bed during treadmill exercise and in an isolated gracilis muscle preparation. Arteriolar vasodilation during exercise, vascular responsiveness and the contributions of sodium retention, sympathetic activity and angiotensin II to altered arteriolar behavior will be examined. Skeletal muscle biopsies and dichloroacetate will be used to study muscle enzymatic changes and the contribution of lactate to exercise intolerance. These studies should help to clarify the mechanism responsible for the reduced maximal exercise capacity of patients with heart failure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
1R01HL034834-01A1
Application #
3348229
Study Section
Respiratory and Applied Physiology Study Section (RAP)
Project Start
1986-06-01
Project End
1989-05-31
Budget Start
1986-06-01
Budget End
1987-05-31
Support Year
1
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
Schools of Medicine
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Wilson, J R; Mancini, D M (1993) Factors contributing to the exercise limitation of heart failure. J Am Coll Cardiol 22:93A-98A
Mellow, E; Redei, E; Marzo, K et al. (1992) Effect of chronic left ventricular failure on beta-endorphin. J Appl Physiol 73:2675-80
Wilson, J R; Coyle, E F; Osbakken, M (1992) Effect of heart failure on skeletal muscle in dogs. Am J Physiol 262:H993-8
Marzo, K P; Frey, M J; Wilson, J R et al. (1991) Beta-adrenergic receptor-G protein-adenylate cyclase complex in experimental canine congestive heart failure produced by rapid ventricular pacing. Circ Res 69:1546-56
Wilson, J R; Lanoce, V; Frey, M J et al. (1990) Arterial baroreceptor control of peripheral vascular resistance in experimental heart failure. Am Heart J 119:1122-30
Mancini, D M; Schwartz, M; Ferraro, N et al. (1990) Effect of dobutamine on skeletal muscle metabolism in patients with congestive heart failure. Am J Cardiol 65:1121-6
Mancini, D M; Coyle, E; Coggan, A et al. (1989) Contribution of intrinsic skeletal muscle changes to 31P NMR skeletal muscle metabolic abnormalities in patients with chronic heart failure. Circulation 80:1338-46
Wilson, J R; Mancini, D M; McCully, K et al. (1989) Noninvasive detection of skeletal muscle underperfusion with near-infrared spectroscopy in patients with heart failure. Circulation 80:1668-74
Frey, M J; Lanoce, V; Molinoff, P B et al. (1989) Skeletal muscle beta-receptors and isoproterenol-stimulated vasodilation in canine heart failure. J Appl Physiol 67:2026-31
Wilson, J R; Frey, M J; Mancini, D M et al. (1989) Sympathetic vasoconstriction during exercise in ambulatory patients with left ventricular failure. Circulation 79:1021-7

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