Abstract
Materials and methods Nine female and male Beagle dogs (age 1.5–3 years, body weight 10 – 15 kg) were anesthetized (neuroleptic anesthesia with droperidol/fentanyl) and artificially ventilated (N2O/O2) [2]. Hemodynamic parameters systolic and diastolic arterial blood pressure (BPS, BPD), left ventricular systolic and end diastolic pressure (LVP, LVEDP), left ventricular dP/dt (LVdP/dt), cardiac output (CO), central venous pressure (CVP), and heart rate (HR) were measured continuously. Total peripheral resistance (TPR) was calculated as mean arterial pressure (BPM) divided by cardiac output. ECG was recorded with standard lead II and RR, PQ, QRS, and QT interval were evaluated. QT was corrected for heart rate by Fridericia's formula (QTcF). Groups of n = 3 dogs received 3 cumulative infusion steps of placebo (1 mM Tris buffer at pH 8.6–8.8 in saline, 0.44–0.67–3.33 ml/kg/h) or BAY 58–2667 at low (1–5– 25 μg/kg/h) or at high (5–15–45 μg/kg/h) infusion rates. Infusion rates were consecutively increased every hour followed by a 2 hour washout period after stop of the final infusion step.
Highlights
BAY 58–2667 is a novel activator of the soluble guanylyl cyclase with vasodilatory properties in diseased blood vessels [1]
Within the scope of a Safety Pharmacology study, effects on cardiovascular function and ECG were examined in anesthetized Beagle dogs after intravenous administration
Cardiovascular function BAY 58–2667 caused a plasma concentration dependent reduction of LVEDP (-98%) and central venous pressure (CVP) (-54%) followed by a vasodilation which was accompanied by counter regulation with increase of heart rate (HR) (+113%) and LV dP/dt (+21%) as a consequence of sympathetic activation
Summary
BAY 58–2667 is a novel activator of the soluble guanylyl cyclase (sGC) with vasodilatory properties in diseased blood vessels [1]. BAY 58–2667 is currently under clinical development for the treatment of acute decompensated heart failure. Within the scope of a Safety Pharmacology study, effects on cardiovascular function and ECG were examined in anesthetized Beagle dogs after intravenous administration. Infusion rates of this placebo-controlled study were chosen to cover approximately the 10 fold of therapeutic plasma levels
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