Different response of the rat left and right heart to norepinephrine

The in vivo hemodynamic and morphologic responses of the rat left (LV) and right (RV) ventricle to continuous long-term i.v. infusion of norepinephrine (NE) at different dosages and for different durations of infusion were studied. Female Sprague-Dawley rats received continuous intravenous infusion of norepinephrine from infors(R) syringe pumps for 24, 48 and 72 h at a dose of 200 mu g . kg(-1) . h(-1). Furthermore, NE was infused for 72 h at dosages of 50, 100 and 200 mu g . kg(-1) . h(-1). The beta-adrenergic blocker and vasodilator with alpha(1)-blocking activity carvedilol (0.5 mg . kg(-1) . h(-1)) was coinfused with NE for 72 h. The hemodynamic effects were measured on intact, anesthetized rats with special Millar(R) ultraminiature pressure tip catheters, and the weights of the left and right ventricles were measured. NE increased heart rate at any time or dose, whereas cardiac output and total peripheral resistance remained unchanged. LV and RV dP/dt(max) were nearly doubled as compared to control values and RVSP was elevated by more than 100%. The effect of NE on LVSP was much less pronounced (< 20%) and only significant at 50 mu g . kg(-1) . h(-1) for 72 h. Neither LV nor RV end-diastolic pressures were elevated, indicating that cardiac failure had not occurred. The LV developed hypertrophy with an increase of the ventricular weight/body weight ratio (LVW/BW) of 22% even after only 2 days of NE (200 mu g . kg(-1) . h(-1)). The RV showed no hypertrophy at any time of the experiments. The NE-induced changes in HR, dP/dt(max), RVSP and LVW/BW were completely prevented by the coinfusion of carvedilol. These studies show that the hemodynamic responses to continuous infusion of NE are more pronounced in the RV than in the LV. Conversely, NE induced hypertrophy only in the LV, not in the RV. The hemodynamic effects of chronic NE infusion did not change significantly between 1 and 3 days of infusion, The in vivo responses to exogenous NE therefore were unaffected by adaptive effects such as downregulation of adrenergic receptors.