Haemodynamic Monitoring

Abstract

The synthesis of adenosine triphosphate (ATP) depends on the coordinated interaction of oxygen delivery and glucose breakdown in the Krebs cycle. Cellular oxygen depots are non-existent, therefore the peripheral cells are totally dependent on the circulation for sufficient oxygen delivery. Shock is the clinical manifestation of cellular oxygen craving. The commonly measured variables — blood pressure, heart rate, urinary output, cardiac output and systemic vascular resistance — are not sensitive or accurate enough to warn of impending death in acutely ill patients nor are they appropriate for monitoring therapy. Calculated oxygen transport and oxygen consumption parameters provide the best available measures of functional adequacy of both circulation and metabolism. In order to optimise oxygen delivery (DO₂), 4 interacting factors must be taken into account: cardiac output, blood haemoglobin content, haemoglobin oxygen saturation and avidity of oxygen binding to haemoglobin. For viscosity reasons, the optimal haemoglobin concentration is in the vicinity of 90 to 100 g/L, but for optimising the oxygen transport 100 to 115 g/L or a haematocrit of 30 to 35% seems better. The p50 (the pO₂ at which haemoglobin is 50% saturated) describes the oxygen-haemoglobin dissociation curve; normally its value is ± 27mm Hg. It can be influenced by attaining normal body temperature, pH, pCO₂ and serum phosphorous levels. In order to obtain an arterial blood saturation (SaO₂) of more than 90% with acceptable haemodynamics, the ventilation mode and inspired oxygen fraction (F_iO₂) must be adapted; care must be taken not to stress the labile circulation with haemodynamic compromising ventilation techniques [e.g. high positive end expiratory pressure (PEEP) levels, inverse-ratio ventilation, etc.]. The factor most amenable to manipulation is the cardiac output, with its 4 determinants — preload, afterload, contractility and heart rate. In daily clinical practice, heart rate should be between 80 and 120 beats/min; small variations are acceptable. Important deviations must be treated by chemically [isoprenaline (isoproterenol)] or electrically (pacing techniques) accelerating the heart, or with the different antiarrhythmic drugs. A wide variety of agents is available to decrease the preload: diuretics [especially furosemide (frusemide)], venodilators like nitroglycerin (glyceryl trinitrate), isosorbide dinitrate (sorbide nitrate) and sodium nitroprusside, ACE inhibitors, phlebotomy, and haemofiltration techniques (peritoneal or haemodialysis, continuous arteriovenous haemofiltration). To increase the preload, volume loading using a rigid protocol (‘rule of 7 and 3’), preferably with colloids, or vasopressor agents [norepinephrine (noradrenaline), epinephrine (adrenaline), dopamine] are useful. Arterial vasopressors are needed to improve perfusion pressure of ‘critical’ (coronary and cerebral) arteries. Afterload can be decreased by arterial vasodilators. Predominantly arterial dilators are hydralazine and clonidine, while sodium nitroprusside, nitroglycerin and isosorbide dinitrate have combined arterial and venous dilating actions. Norepinephrine, epinephrine and dopamine combine inotropic with vasoconstricting properties; dobutamine, dopexamine and the phosphodiesterase inhibitors amrinone, milrinone and enoximone are combined positive inotropic and afterload reducing drugs. The phosphodiesterase inhibitors possess lusitropic (i.e. promoting myocardial relaxation) effects. Myocardial oxygen consumption is certainly increased by norepinephrine, epinephrine, isoprenaline and dopamine, while dobutamine only has minimal effects and the phosphodiesterase inhibitors lower it. To treat a critically ill patient according to the abovementioned strategy, the intensive care physician must rely on invasive haemodynamic measurements. Several derived parameters, all critically dependent on a correct determination of the cardiac output, give insight into pathophysiological process; they are also necessary to guide sometimes complex pharmacological manipulations in order to maximise oxygen delivery and consumption.