Abstract
PurposeCrystalloid fluid and vasoactive drugs are used in the early treatment of sepsis. The purpose of the present study was to examine how these drugs alter plasma volume expansion, peripheral edema, and urinary excretion.MethodsTwenty-five anesthetized sheep were made septic by cecal puncture and a short infusion of lipopolysaccharide. After 50 min, a slow infusion of isotonic saline was initiated: the saline either contained no drug, norepinephrine (1 μg/kg/min), phenylephrine (3 μg/kg/min), dopamine (50 μg/kg/min), or esmolol (50 μg/kg/min). Ten min later, 20 mL/kg Ringer´s lactate solution was given over 30 min. Central hemodynamics, acid-base balance, and the urinary excretion were monitored. Frequent measurements of the blood hemoglobin concentration were used as input in a kinetic analysis, using a mixed effects modeling software.ResultsThe fluid kinetic analysis showed slow distribution and elimination of Ringer´s lactate, although phenylephrine and dopamine accelerated the distribution. Once distributed, the fluid remained in the peripheral tissues and did not equilibrate adequately with the plasma. Overall, stimulation of adrenergic alpha1-receptors accelerated, while beta1-receptors retarded, the distribution and elimination of fluid. A pharmacodynamic Emax model showed that Ringer´s lactate increased stroke volume by 13 ml/beat. Alpha1-receptors, but not beta1-receptors, further increased stroke volume, while both raised the mean arterial pressure. Modulation of the beta1-receptors limited the acidosis.ConclusionsStimulation of adrenergic alpha1-receptors with vasoactive drugs accelerated, while beta1-receptors retarded, the distribution and elimination of fluid. The tendency for peripheral accumulation of fluid was pronounced, in particular when phenylephrine was given.
Highlights
Crystalloid fluid loading and the administration of vasoactive drugs are essential steps in the early treatment of septic patients with suspected hypovolemia and tissue hypoperfusion [1, 2]
A pharmacodynamic Emax model showed that Ringers lactate increased stroke volume by 13 ml/beat
If the hypovolemia and hypotension is not resolved by volume loading, the treatment should be augmented by administration of norepinephrine, phenylephrine, or dopamine [3, 4]
Summary
Crystalloid fluid loading and the administration of vasoactive drugs are essential steps in the early treatment of septic patients with suspected hypovolemia and tissue hypoperfusion [1, 2]. If the hypovolemia and hypotension is not resolved by volume loading, the treatment should be augmented by administration of norepinephrine, phenylephrine, or dopamine [3, 4]. Vasoactive drugs markedly change the distribution and elimination of crystalloid fluid, thereby altering the plasma volume expansion, urinary excretion, and the risk of peripheral edema [5]. The interactions between fluid and vasoactive drugs have not been studied with respect to sepsis. This type of study is of potential importance in the search for optimal combinations of crystalloids and vasoactive agents
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