Acute Cardiovascular Effects of Magnesium and Their Relationship to Systemic and Myocardial Magnesium Concentrations after Short Infusion in Awake Sheep

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Vol. 297, Issue 3, 1176-1183, June 2001

Acute Cardiovascular Effects of Magnesium and Their Relationship to Systemic and Myocardial Magnesium Concentrations after Short Infusion in Awake Sheep

D. Zheng, R. N. Upton, G. L. Ludbrook and A. Martinez

Anaesthesia and Intensive Care, Royal Adelaide Hospital/University of Adelaide, North Terrace, Adelaide, Australia

	Abstract

Top Abstract Introduction Materials and Methods Results Discussion References

The temporal relationship between the systemic and myocardial concentrations of magnesium and some of its acute cardiovasculareffects were examined after short i.v. infusion administrationof magnesium (30 mmol over 2 min) in five awake chronically instrumentedsheep. Magnesium decreased mean arterial blood pressure and systemicvascular resistance (SVR) by 23 and 41% from baseline, respectively.These hemodynamic changes were consistent with magnesium producingprimary reductions in SVR with partial heart rate (HR)-mediatedcompensation of blood pressure. Cardiac output and HR increasedby 38 and 38% from baseline, respectively. Magnesium had littleeffect on myocardial contractility, but substantially increasedmyocardial blood flow (MBF, 77% above baseline) primarily dueto direct myocardial vasodilation. The peak arterial and coronarysinus serum magnesium concentrations were 6.94 ± 0.26 (mean ±S.E.M.) and 6.51 ± 0.20 mM, respectively, at 2 min. Both arterialand coronary sinus magnesium concentrations at the end of thestudy were still more than 3 mM, whereas all the cardiovasculareffects were back to baseline. The myocardial kinetics of magnesiumwas consistent with rapid equilibration of magnesium (half-life0.4 min) with a small distribution volume (71 ml) consistent withthe extracellular space of the heart. In conclusion, magnesiumwas shown to have a rapid equilibration between the plasma/serumconcentrations of magnesium and its extracellular concentrationin the myocardium. However, the primary cardiovascular effectof magnesium (reductions in SVR) preceded its extracellular concentrations,and was a direct function of its arterial concentration. A "threshold"model for changes in SVR was preferred when linked to the arterialmagnesiumconcentration.

	Introduction

Top Abstract Introduction Materials and Methods Results Discussion References

Intravenous magnesium has been increasingly used to treat and prevent many acute cardiovascular diseases (Altura and Altura,1985; Nattel et al., 1991; Hampton et al., 1994; Miller et al.,1995; Fawcett et al., 1999). Functionally, magnesium can be regardedas a cardiovascular drug with calcium antagonistic and antiadrenergicproperties (James, 1992). Its cardiovascular effects include directand indirect dilatation of blood vessels, an antiarrhythmic effect,and possibly myocardial depression. Although it is known thatthere is a direct relationship between magnesium plasma/serumconcentration and cardiovascular effects at near steady state(Friedman et al., 1987; James et al., 1987; Nakaigawa et al.,1997), the relationship between the time courses of concentrationand effect is poorly understood. Increased knowledge of this temporalrelationship may provide a more rational basis for the designof acute intravenous dose regimens of magnesium for the managementof cardiovascularsymptoms.

There are several issues that need to be resolved before this can be done. First, there is some ambiguity in the literatureon the effects of magnesium on some cardiovascular variables suchas myocardial contractility and myocardial blood flow, which maybe due to differences in magnesium dose and experimental conditionsbetween studies. Second, it is not known to what extent the plasma/serumconcentrations of magnesium reflect the concentration of magnesiumin important organ systems mediating the cardiovascular effects(e.g., blood vessel walls for vasodilatation, and the myocardiumfor direct effects on contractility and the ECG). Third, it isunclear whether the cardiovascular effects of magnesium are mediatedby its extracellular or intracellular concentration, or a combinationof both (Murphy et al., 1991) in theseorgans.

We have previously examined the relationship between the myocardial pharmacokinetics and dynamic of a number of drugs in sheep(Huang et al., 1993a; Upton et al., 1996, 1999), and in this studyapplied these methods to intravenous magnesium to address someof these issues. The aims of the study were as follows. 1) Todefine the time course of some of the cardiovascular effects ofmagnesium after an intravenous infusion of 30 mmol of magnesiumsulfate over 2 min to conscious, instrumented sheep. Myocardialcontractility and myocardial blood flow were measured in a closedchested, conscious preparation without concurrent drugs followinga high dose of magnesium to deduce the effect of magnesium aloneon these cardiovascular variables. 2) To define the time courseof the systemic and myocardial concentrations of magnesium, withthe latter inferred from the concentration of magnesium in coronarysinus blood leaving the heart. Modeling of myocardial kineticswas used to test the hypothesis that the extracellular magnesiumconcentration in the heart could be deduced from this coronarysinus concentration (i.e., consistent with venous equilibrationof the extracellular space). 3) To examine the temporal relationshipbetween systemic and myocardial concentrations of magnesium andkey cardiovascular effects using kinetic-dynamicmodeling.

	Materials and Methods

Top Abstract Introduction Materials and Methods Results Discussion References

General Experimental Preparation

The study was approved by the Animal Ethics Committee of the University of Adelaide. The sheep were prepared in two steps.About 2 weeks before experimentation, sheep (2-3 years of ageand approximately 50 kg) were anesthetized with i.v. thiopental(1.5 g) and the trachea intubated with a cuffed tracheal tube(9 mm i.d.; Sheridan Catheter Corp., Argyle, NY). Anesthesia wasmaintained with 2% halothane and 100% oxygen and end-expiratorycarbon dioxide was monitored using a capnograph (Cardiocap; InstrumentariumCorp, Helsinki, Finland) and kept between 35 and 40 mmHg.

The right femoral artery and vein were exposed via a groin incision. Using the Seldinger technique (Runciman et al., 1984),a 7-French and a 9-French gauge catheter (Multi-purpose A1 catheter;Cook Australia, Brisbane, Australia) were placed in the abdominalaorta. Through the femoral vein, an 8.5-French introducer catheter(Biosensors International Pty Ltd, Singapore) was placed in theinferior vena cava (IVC). Through the introducer catheter, a 7.5-Frenchmultilumen thermodilution catheter (Swan-Ganz, Biosensors InternationalPte Ltd) was placed in the pulmonary artery. The position of theSwan-Ganz catheter was confirmed by monitoring the pressure wavepattern with a pressure transducer (model 4-327-I; Bell and HowellInc., Pasadena, CA) during catheter advancement (Runciman andLudbrook, 1993).

Two days later, the sheep were anesthetized as described above for probe placement and further catheterization using a modificationof the method reported previously (Huang et al., 1992). A leftthoracotomy at the 4th intercostal space and a pericardiotomywere performed to expose the left main coronary artery and thepulmonary artery. Doppler flow probes (Titronics Medical Instruments,Iowa City, IA) were placed around the left main stem coronaryartery (for measurement of an index of left coronary blood flow)and pulmonary artery (for measurement of cardiac output, CO).The probes were secured around the arteries with cotton tape,which acted as a "cuff" around the arteries and ensured a constantvessel caliber. The apex of the heart was stitched with a 2-0silk suture, a micro transducer (Codman MicroSensor; Johnson &Johnson Professional, Inc., Raynham, Miami, FL) was placed 3 cminto the left ventricle through a 5-gauge needle via the apexof heart and fixed securely with the suture. The hemiazygous vein,which drains into the coronary sinus of sheep, was ligated outsidethe pericardium, to ensure the coronary sinus contained pure effluentblood from the myocardium. The leads of the probes and the microtransducer were exteriorized although the chest incision and asubdermaltunnel.

The right jugular vein was exposed via a neck incision. A 7-French gauge (B1; Cordis Corporation, Miami, FL) was place intothe coronary sinus to sample efferent blood from the myocardium.The position of the catheters was confirmed under direct visionusing a fluoroscope with the injection of radio-opaque contrast(Conray 420; May and Baker Ltd, Dagenham, UK) into the coronarysinus. All the surgical procedures were carried out with usingsterile technique and all incisions were closed. The sheep wererecovered from anesthesia and housed in metabolic crates withfree access to food and water. All catheters were flushed at leastevery 2 days with heparinized (50 IU/ml) 0.9%saline.

Cardiovascular Measurements

During the experiments, the Doppler frequency shifts from both the coronary artery and pulmonary artery Doppler flow probeswere recorded at a sampling rate of 1 Hz using a four-channelpulsed Doppler flowmeter (Bioengineering, University of Iowa,56 M.R.F, Iowa City, IA) and an analog-to-digital card (MetraByteDAS 16-G2; MetraByte Corp., Taunton, Miami, FL) in a personalcomputer (Microbits 486-based IBM compatible). These were usedas indices of myocardial blood flow and cardiac output, respectively.It has been shown that the left coronary artery blood flow velocitywas representative of flow in a region corresponding to 77% ofthe heart (Huang et al., 1993b). The pulmonary artery Dopplerflow probes were calibrated in vivo by correlating the Dopplershifts with cardiac output measured intermittently using a thermodilutiontechnique (Huang et al., 1992).

Mean arterial pressure (MAP) and central venous pressure (CVP) were measured using a pressure transducer on an arterial catheterand an IVC catheter, respectively. Left ventricular pressure,MAP, and CVP were recorded using the same data acquisition system.The peak value of the increasing rate of pressure rise of theleft ventricle (LV dP/dt_max) was calculated and used as an indexof myocardial contractility. Heart rate (HR) was also calculatedfrom the pressure wave of the leftventricle.

Myocardial oxygen consumption (MVO₂) was calculated as the product of myocardial blood flow (MBF, assuming a baseline flowof 122 ml/min; Huang et al., 1992) and the arteriocoronary sinusoxygen content gradient. Systemic vascular resistance (SVR) wascalculated as the difference between MAP and CVP (mm Hg) overCO (l/min) and is reported in resistance units (mm Hg min l¹).

Experimental Design

Studies were conducted in five sheep prepared as described above. On the experimental day, the sheep remained in their metaboliccrates with their weight supported by a sling to minimize sheepmovement. A study was not commenced until at least 40 min afterthe placement of the hemodynamic measurement devices, and thehemodynamic measurements had been stable for approximately 10min. After 5 min of baseline hemodynamic measurements, 30 mmolof magnesium sulfate was infused intravenously via the IVC catheterover 2 min (0.6 mmol/kg). The start of the infusion was designatedtime zero. Arterial and femoral venous blood samples (5 ml) weretaken at 0, 1, 2, 4, 10, and 25 min for serum magnesium assay,and were assayed using a Ektachem 700 analyzer (Kodak GmbH, Stuttgart,Germany). Blood was also sampled from arterial and coronary cathetersat 0, 2, and 25 min after commencement of administration of magnesiumfor blood gas analysis (ABL Radiometer Medical A/S, Copenhagen,Denmark) to determine blood oxygen tension (pO₂), pH, blood carbondioxide tension (pCO₂), and blood oxygen saturation (SO₂).

Data Analysis

Modeling of Myocardial Kinetics. Hybrid modeling (Upton, 1996; Upton et al., 2000) was used to examine the ability of various kinetic models to describe theobserved magnesium concentrations in coronary sinus blood. Modelswere constructed as a series of differential equations with theScientist for Windows software package (version 2; Micromath ScientificSoftware, Salt Lake City, UT), and were fitted to mean data forthe five sheep after initial analysis showed little interindividualvariation in magnesium concentrations. The measured arterial magnesiumconcentrations (C_art) and blood flow entering the heart were fittedto forcing functions (exponential and polynomial functions, respectively)and these were used as the input functions for the myocardialkinetic models. The measured coronary concentrations (C_cs) wereused to estimate the parameters of the models by curve fitting.Curve fitting was by a least-squares method based on the maximizationof model selection criteria (MSC) of the Scientist program (Upton,1996; Upton et al., 2000). Three models were examined as outlinedbelow, where Q_h is myocardial blood flow, and V_h is the apparentvolume of magnesium in themyocardium.

A single flow-limited compartment model:

V<UP>h</UP> · <FR><NU><UP>d</UP>C<UP>cs</UP></NU><DE><UP>d</UP>t</DE></FR>=Q<UP>h</UP> · (C<UP>art</UP>−C<UP>cs</UP>) (1)

A single flow-limited compartment with first order loss model:

V<UP>h</UP> · <FR><NU><UP>d</UP>C<UP>cs</UP></NU><DE><UP>d</UP>t</DE></FR>=Q<UP>h</UP> · (C<UP>art</UP>−C<UP>cs</UP>)−k<UP>loss</UP> · C<UP>cs</UP> (2)

where k_loss governs the rate of the loss and has the units of volume per unittime.

A membrane-limited compartment model. In this model, "PS" is used to represent membrane permeability, and C_deep is the magnesium concentration in the deep compartmentof the myocardium with a volume given by V_deep:

V<UP>h</UP> · <FR><NU><UP>d</UP>C<UP>cs</UP></NU><DE><UP>d</UP>t</DE></FR>=Q<UP>h</UP>(C<UP>art</UP>−C<UP>cs</UP>)+<UP>PS</UP> · (C<UP>deep</UP>−C<UP>cs</UP>) (3)

V<UP>deep</UP> · <FR><NU><UP>d</UP>C<UP>deep</UP></NU><DE><UP>d</UP>t</DE></FR>=<UP>PS</UP> · (C<UP>cs</UP>−C<UP>deep</UP>)

A graphical representation of the three kinetic models is shown in Table 2.

Kinetic-Dynamic Modeling. SVR was considered the primary cardiovascular parameter affected by magnesium. Four dynamic models were examined that relatedthe arterial or coronary sinus magnesium concentrations (C) tothis effect:

Linear Model. A simple linear relationship between concentration and effect, defined by the slope and intercept of a line:

<UP>SVR</UP>=<UP>slope</UP> · C+<UP>intercept</UP> (4)

Linear Model with Delay. As for the first model, but SVR was related to magnesium concentration in a hypothetical effect compartment whose time courseof concentrations was delayed relative to the measured concentrationas given by the rate constant k_eo. The rateconstant was constrainedduring fitting to be between 0 and 100 min¹. C_eff is the effect compartment concentration:

<FR><NU><UP>d</UP>C<UP>eff</UP></NU><DE><UP>d</UP>t</DE></FR>=k<UP>eo</UP> · (C−C<UP>eff</UP>)

<UP>SVR</UP>=<UP>slope</UP> · C<UP>eff</UP>+<UP>intercept</UP> (5)

A Linear Model with a Threshold. This model was the same as the linear model, but SVR was unchanged from baseline (SVR_base) below a threshold (T) concentration:

<UP>If</UP> C<T, <UP>then SVR</UP>=<UP>SVRbase</UP>

<UP>If</UP> C>T, <UP>then SVR</UP>=<UP>slope</UP> · C+<UP>intercept</UP> (6)

<UP>intercept</UP>=<UP>SVR</UP><UP>base</UP> − T · C

A Tolerance Model. This model was adapted from that used by Ekblom et al. (1993) to describe tolerance to morphine, and was such that the effectsof magnesium on SVR could become less with time, even if the magnesiumconcentrations were held constant. This type of model can empiricallyaccount for a variety of mechanisms of tolerance (Mandema andWada, 1995). Conceptually, the changes in SVR from baseline (SVR_base)can be thought of as the net result of a reduction attributedto the effect of magnesium (SVR_e), and an increase due to thedevelopment of tolerance (SVR_t):

<UP>SVR</UP>=<UP>SVR</UP><UP>base</UP> − <UP>SVR</UP><UP>e</UP> + <UP>SVRt</UP> (7)

The direct effect of magnesium was linearly related to concentration:

The tolerance was related to concentrations in a hypothetical tolerance compartment, which could be delayed relative to themeasured concentration, as given by the rate constant k_t0:

<UP>d</UP>C<UP>tol</UP>/<UP>d</UP>t=k<UP>t0</UP> · (C−C<UP>tol</UP>)

<UP>SVR</UP><UP>t</UP> = <UP>slope</UP><UP>t</UP> · C<UP>tol</UP>

Statistical Analysis

To compare the effect of magnesium on MAP, SVR, CO, MBF, LV dP/dt_max, HR, pH, pCO₂, pO₂, SO₂, and MVO₂, measurements wereexpressed as a percentage of baseline, and then the mean and 95%confidence limits were calculated. If the mean and its 95% confidencelimits of a measured value lay outside the 95% confidence limitsof the baseline data, the value was recorded as being statisticallysignificant. Paired t tests were used to compare the arterialand coronary sinus magnesium concentrations. p < 0.05 was recordedas statisticallysignificant.

	Results

Top Abstract Introduction Materials and Methods Results Discussion References

Cardiovascular and Other Effects of Magnesium. Magnesium caused minor respiratory depression, as indicated by transient reductions in arterial pO₂ and SO₂, and increasesin arterial pCO₂ (Table 1). The increase of arterial pCO₂ at2 min was 29% above baseline.

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TABLE 1
Arterial and coronary sinus pH, pCO₂, pO₂, and SO₂ at baseline, 2 and 25 min in five sheep
Data are shown as mean (95% confidence limits) and letters indicate significant difference when observed value and its expected 95% confidence limits were outside the confidence limits of the baseline data.

There were no significant changes in the time course of LV dP/dt_max (Fig. 1A), indicating that magnesium was not a myocardialdepressant in this experimental paradigm.

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Fig. 1. Time courses of dP/dt_max (A) and MBF (B). Magnesium was administrated at time = 0 for 2 min. Data are shown as the mean (symbols) and 95% confidence limits (dashed line). The 95% confidence limits of the baseline data are shown as the solid lines. At any particular time, a statistically significant difference occurs if the observed value and its 95% confidence intervals lay outside of 95% confidence interval of the baseline period.

During and shortly after the infusion of magnesium, there was a substantial increase in MBF from baseline, with a peak increaseof 77% at 1 min (Fig. 1B). However, there were no significantchanges in MVO₂. The values of MVO₂ at baseline, and 2 and 25min after the infusion (mean and 95% confidence limits) were 4.4(3-5.7), 3.9 (3.3-4.6), and 3.6 (2.7-4.6) ml/min/100 g, respectively.Increased MBF in the face of unchanged MVO₂ is consistent withthe observation that the coronary sinus SO₂ was significantlyincreased above baseline at 2 min (Table 1). Overall, the increasein MBF caused by magnesium appears to be due to a direct vasodilatoryeffect on the coronary blood vessels, rather than secondary tocardiovascular changes that increase myocardial work and thereforeMVO₂.

There were significant reductions in MAP and SVR from baseline (Fig. 2, A and B), with peak reductions of 23 and 41% for each,respectively, at 2 min. This was accompanied by an increase inCO (Fig. 3A) and HR (Fig. 3B), with a peak increase of 38% at2 min for both parameters. Stroke volume (SV) was essentiallyunchanged (Fig. 3C). This pattern of hemodynamic changes is consistentwith magnesium-dependent reductions in SVR, with partial compensationof MAP decreases via reflex increases in heart rate. Increasesin preload due to a transient fluid shift from the arterial tovenous circuit may also have contributed to the increase in CO,although preload was not measured in the present study. In subsequentkinetic dynamic analysis, a reduction in SVR was considered tobe the primary cardiovascular effect of magnesium, and it wasthis effect that was related to the measured magnesium concentrations.

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Fig. 2. Time courses of MAP (A) and SVR (B). Magnesium was administrated at time = 0 for 2 min. Data are shown as the mean (symbols) and 95% confidence limits (dashed line). The 95% confidence limits of the baseline data are shown as the solid lines. At any particular time, a statistically significant difference occurs if the observed value and its 95% confidence intervals lay outside of 95% confidence interval of the baseline period.

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Fig. 3. Time courses of cardiac output (CO) (A), HR (B), and SV (C). Magnesium was administrated at time = 0 for 2 min. Data are shown as the mean (symbols) and 95% confidence limits (dashed line). The 95% confidence limits of the baseline data are shown as the solid lines. At any particular time, a statistically significant difference occurs if the observed value and its 95% confidence intervals lay outside of 95% confidence interval of the baseline period.

Myocardial Pharmacokinetics of Magnesium. The observed arterial and coronary sinus blood concentrations of magnesium are shown in Fig. 4. There was a significant differencebetween arterial and coronary sinus concentration at 1 min afterthe start of the infusion. There was a general trend for uptakeof magnesium into the heart (arterial > coronary sinus concentrations)for approximately 10 min after the start of the infusion.

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Fig. 4. Time course of observed mean arterial ( $open circle$ ) and coronary sinus (

) concentrations. Magnesium was administrated at time = 0 for 2 min. Data are shown as mean and S.E.M. The mean observed (symbols) and predicted coronary sinus concentrations for the flow-limited model (solid line) are also in the inset.

The goodness of fit of the models of myocardial magnesium kinetics and their parameter values are shown in Table 2. The flow-limitedmodel was the best fit of the data; the line of best fit to thecoronary sinus magnesium concentrations is shown in the insetof Fig. 4. The membrane-limited model collapsed to a flow-limitedmodel, as indicated by very small values of PS and V_deep, whereasthe flow-limited model with a first order loss returned a lowand uncertain value for the k_loss.

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TABLE 2
Goodness of fits of the model of magnesium kinetics in the myocardium
For MSC, the higher the number, the better the fit. The model parameters were apparent distribution volume (V_h), first order loss (k_loss), membrane permeability (PS), and deep compartment (V_deep) in myocardium. The data are shown as the mean and (S.D.).

The good fit of the flow-limited model is consistent with the concept of a distribution volume of magnesium in the heart (approximately71 ml) that is in equilibrium with coronary sinus blood. Thisvolume can be compared with the true volume of the region of theheart drained by the coronary sinus catheter (233 g in sheep;Huang et al., 1993b

), and therefore represents approximately 30%of the total mass of the region of the heart under study. Thisdistribution volume can also be compared with the baseline myocardialblood flow (122 ml/min; Huang et al., 1992

); the half-time forequilibration of the volume with serum was therefore 0.40min.

Pharmacokinetic-Pharmacodynamic Relationships. The parameters' values of the various dynamic models and their MSC values are shown in Table 3. The linear dynamic modelproduced an acceptable fit of the SVR data when linked to thearterial concentrations (Fig. 5), but was less successful whenlinked to the coronary sinus concentrations (Table 3). Addingan effect delay to either did not improve the fit, and producedestimates of k_eo that were equal to the upper constraint (100min¹). This value of k_eo produced time course of measured concentrationand effect compartment concentration that were essentially identical.Overall, the data suggest that the arterial magnesium concentrationswere directly related to the reductions in SVR with no time delay,and that the time course of the coronary sinus concentrationslag behind both the time course of the arterial concentrationsand reductions in SVR.

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TABLE 3
Goodness of fits of the dynamic models
For MSC, the higher the number, the better the fit. The class leader for each site has been highlighted in bold.

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Fig. 5. Kinetic-dynamic relationship for the linear effect model. The solid circles are the observed time course of the arterial magnesium concentration. Data are shown as mean and S.E.M. The open circles are the observed time course of SVR. Data are shown as the mean (symbols) and 95% confidence limits (dashed line). The solid line is the line of best fit of the linear effect model linked to the arterial magnesium concentrations.

Close inspection of Fig. 5 will show that the greatest discrepancy between the line of best fit for the linear model and theSVR data occurs for the last time point (25 min), although thisis also the value of SVR with the widest 95% confidence intervals.The application of threshold and tolerance models to the datawere an attempt to account for this discrepancy, which is consistentwith SVR returning to near baseline while the magnesium concentrationsremained elevated (Figs. 2B and 4). The threshold model was preferredwhen linked to the arterial concentration, whereas the tolerancemodel was preferred when linked to the coronary sinus concentrations,but returned an uncertain value for the tolerance rate constant(k_tol). This suggests that the threshold dynamic model was suitablefor describing the relationship between the arterial magnesiumconcentration and SVR.

	Discussion

Top Abstract Introduction Materials and Methods Results Discussion References

Cardiovascular Effects of Magnesium. The pattern of hemodynamic changes observed was consistent with peripheral vasodilatation, hypotension, and a reflex increasein CO, predominantly due to an increase in HR. The use of an awakepreparation avoided any anesthetic depression of autonomic reflexesor myocardial function that may complicate the interpretationof some earlier studies (Friedman et al., 1987). The changes observedwere similar to those previously reported in studies using lightlyanesthetized baboons (James et al., 1987), although decreasesin HR were more common in studies where magnesium concentrationsreached supratherapeutic concentrations (Nakaigawa et al., 1997).

Myocardial Contractility. There was no evidence of myocardial depression, as determined by LV dP/dt_max, despite magnesium concentrations reaching around7 mM, although it is possible a small direct myocardial depressanteffect may have been countered by a reflex sympathetic responseto hypotension. This is consistent with much of the publishedliterature, which generally shows minimal cardiac depression attherapeutic concentrations (in the order of 2-3 times baselinelevels). Critelli et al. (1977) reported that bolus administrationof magnesium in humans produced only small decreases in indicesof myocardial contractility in patients with mild myocardiosclerosis,but more significant decreases in patients with impaired cardiacfunction (New York Heart Association class III-IV). In lightlyanesthetized baboons, magnesium produced minimal myocardial depression,and even at very high magnesium concentrations a decrease in COseemed to be HR mediated (James et al., 1987). Nakaigawa et al.(1997) reported that magnesium produced dose-dependent decreasesin LV dP/dt_max in anesthetized dogs. This depression was, however,minor at blood concentrations similar to those achieved in thecurrent study, but became marked with blood concentrations ofaround 9 to 14 mg/dl. In vitro, Bass et al. (1958) demonstratedusing a modified Langendorff heart preparation that low concentrationsof magnesium (0.025-2.5 mg) did not affect myocardial contractility,whereas higher doses (25-250 mg) temporarily depressed contractility.In contrast, Friedman et al. (1987) found magnesium reduced LVdP/dt_max by around 30% with magnesium concentrations similar tothose in the current study; chloralose anesthesia may have beena contributingfactor.

The use of awake animals in the present study meant that some respiratory depression and mild hypercarbia was induced. Althoughit is possible that hypercarbia influenced the data in the currentstudy, it is known that even very large increases in pCO₂ produceminimal or no changes in CO, LV dP/dt_max, and HR (Larrieu et al.,1978

; Foex and Ryder, 1979

; van den Bos et al., 1979

), suggestingany influence in the current study wasminimal.

Myocardial Blood Flow. Although an increase in MBF would be expected in the present study, considering the large decrease in SVR, MBF is also influencedby the work performed by the heart. This in turn is influenced(broadly) by SV, MAP, and HR. Following the administration ofmagnesium in the present study, MAP decreased whereas HR increased.The overall work of the heart therefore appeared unchanged, inagreement with the unchanged MVO₂. The increase in MBF in theface of unchanged MVO₂ is consistent with the increase in coronarysinus oxygen content. Overall, the data suggest that magnesiumproduced coronary hyperemia due to direct vasodilatation of coronaryblood vessels. This is consistent with the work of Scott et al.(1961) who reported that MBF velocity was almost doubled, andcoronary vascular resistance was decreased, after intracoronaryinfusion of magnesium in the dog heart, and in vitro studies showing,magnesium to have direct coronary vasodilating effects (Bass etal., 1958; Altura and Altura, 1984, 1985). In contrast, Nakaigawaet al. (1997) reported no change in MBF or in CO, but MVO₂ andoxygen extraction bothdecreased.

In the current study, the small decrease in hemoglobin saturation due to magnesium-induced respiratory depression was unlikelyto have affected MBF, but it is possible that the concurrent mildhypercarbia may have had a small influence. Hypercarbia has beenshown to produce increases in MBF (Foex and Ryder, 1979

; van denBos et al., 1979

), and these increases have been shown to exceedincreases in MVO₂ (Foex and Ryder, 1979

; van den Bos et al., 1979

).However these increases have been associated with marked hypercarbia(over 70 mm Hg), and it seems unlikely that the pCO₂ of around45 mm Hg in the current study contributed more than a small degreeto the large (77%) increase in MBF velocity. This is supportedby the observations from pilot studies using the present experimentalpreparation where it was found that increasing inspired CO₂ from0 to 10% had a minimal effect onMBF.

Myocardial Pharmacokinetics of Magnesium. Magnesium ions equilibrate slowly across cell membranes (probably via ion channels). Intracellular concentrations are a functionof complex buffering of magnesium ions with ATP and other moleculeswithin the cell (Raftos et al., 1999). The electrochemical gradientacross the cell membrane drives the flux of extracellular magnesiuminto the cell, but the intracellular concentrations of free magnesiumare much less than expected by this process. The low intracellularconcentration at equilibrium is achieved by relatively slow activetransport of magnesium out the cell via a Na⁺-Mg²⁺ antiports (Flatman, 1991).

The kinetic modeling supports the notion that this active transport of magnesium out of the cell is sufficient to constrainthe distribution volume of exogenous magnesium to the extracellularspace. The distribution volume was found to be 30% of the massof the region of the heart studied, which includes the blood.The extracellular volume of heart without blood in rat has beenreported to be 15 to 18% of the total volume, depending on themarkers used (Makos et al., 1998

). In addition to the contributionof blood to the distribution volume, there may be some differencesin the binding of magnesium between the serum and interstitialfluid that contributes to the larger volume observed in the presentstudy. Certainly, the data suggest that there is very rapid equilibrationof magnesium between serum and the extracellular space, and thatthe magnesium concentration in venous serum emerging from theheart is representative of its concentration in the extracellularspace. In most circumstances where magnesium is administered moreslowly than in the present study, it would be expected that thetotal serum concentrations of magnesium are representative ofthe total magnesium concentration in the extracellularspace.

Pharmacokinetic-Pharmacodynamic Relationships. Magnesium is known to modify the properties of a number of ion channels in the cell membrane. Although some channels are affectedby the intracellular concentration of magnesium, others (includingits calcium channel blocking effects) are affected by its extracellularconcentration (Murphy et al., 1991; Bara et al., 1993). It wouldseem likely that the reductions in SVR caused by magnesium area function of its calcium channel blocking effects relaxing vascularsmooth muscle. However, the data suggest that the "global" extracellularconcentrations of magnesium, as represented by the effluent concentrationsfrom the heart, do not determine this primary cardiovascular effectof magnesium. The fact that this effect was better related tothe arterial concentrations of magnesium suggest that magnesiumis acting directly on "proximal" segments of the microvasculature,presumably the arterioles responsible for regulating vascularresistance. Capillary permeability theory dictates that the proximalsegments of the exchange microvasculature equilibrate first withthe afferent arterial blood, whereas distal segments equilibratewith efferent venous blood (Stec and Atkinson, 1981).

An interesting finding in the study was that both the arterial and coronary sinus magnesium concentrations at the end of thestudy were more than 3 mM, at which time all the cardiovascularvariables had returned to baseline. A threshold effect was tested,as Bolan et al. (1985)

demonstrated a lack of hemodynamic effectswith blood magnesium concentrations below 4 mM in pregnant sheep.Alternatively, an acute tolerance to the effects of magnesiumwould explain the same observation. The mechanism of tolerancecould take a number of forms, most of which are mathematicallyequivalent to the tolerance model investigated here. For example,serum magnesium exists in two forms: bound to covalent ligands(i.e., plasma proteins) and free ionized magnesium. The free magnesiumfraction in the whole blood is about 59 to 71% (Brookes and Fry,1993

; Ising et al., 1995

; Hafen et al., 1996

). Total serum magnesiumwas measured in the present study, whereas only free ionized magnesiumis thought to have biological activity. Tolerance could be accountedfor by progressive, slow conversion of free to bound magnesiumduring the course of the study. In our own laboratory, we havefound that the vasodilatory effect of magnesium infused directlyinto a muscle bed diminishes with time (Zheng et al., 2000

Implications from the study are first that there is rapid equilibration between the plasma/serum concentrations of magnesiumand its extracellular concentration in the myocardium. It canbe concluded that monitoring arterial concentrations of magnesiumis therefore representative of its extracellular concentrationsin the heart. Second, the primary cardiovascular effects of magnesium(reductions in SVR) were initially related to these arterial concentrations.However, important cardiovascular effects may not be directlyrelated to these concentrations after longer time periods ( $>=$ 25min).

	Acknowledgments

We thank Dr. K. Rowland and staff of the Institute of Medical and Veterinary Science, South Australia for performing the magnesiumassay.

	Footnotes

Accepted for publication February 14, 2001.

Received for publication November 21, 2000.

This research was supported by grants from National Health and Medical Research Council ofAustralia.

Send reprint requests to: Da Zheng, Anesthesia and Intensive Care, The University of Adelaide, Adelaide, Australia, SA 5005. E-mail: da.zheng{at}adelaide.edu.au

	Abbreviations

IVC, inferior vena cava; CO, cardiac output; MAP, mean arterial blood pressure; CVP, central venous pressure; LV dP/dt_max, maximum positive rate of change of left ventricular pressure; HR, heart rate; MVO₂, myocardial oxygen consumption; MBF or Q_h, myocardial blood flow; SVR, systemic vascular resistance; pO₂, blood oxygen tension; pCO₂, blood carbon dioxide tension; SO₂, blood oxygen saturation; MSC, model selection criteria; SV, stroke volume; C_art, arterial magnesium concentration; C_cs, coronary sinus magnesium concentration; V_h, apparent distribution volume of magnesium in the myocardium.

	References

Top Abstract Introduction Materials and Methods Results Discussion References

Altura BM and Altura BT (1984) Magnesium, electrolyte transport and coronary vascular tone. Drugs 28 (Suppl 1): 120-142.
Altura BM and Altura BT (1985) New perspectives on the role of magnesium in the pathophysiology of the cardiovascular system. I. Clinical aspects. Magnesium 4: 226-244[Medline].
Bara M, Guiet-Bara A and Durlach J (1993) Regulation of sodium and potassium pathways by magnesium in cell membranes. Magnesium Res 6: 167-177.
Bass P, Mazurkiewicz I and Melville KI (1958) Effects of magnesium on coronary flow and heart action and its influence on the responses to adrenaline and noradrenaline. Arch Int Pharmacodyn 117: 9-22.
Bolan JC, Craft JB, Jr, Patch JH, Woolf WA, Fabro S, Lahijani J and Mazel P (1985) Pharmacokinetics of magnesium sulfate in the sheep model. Pediatr Pharmacol 5: 189-199.
Brookes CI and Fry CH (1993) Ionised magnesium and calcium in plasma from healthy volunteers and patients undergoing cardiopulmonary bypass. Br Heart J 69: 404-408[Abstract/Free Full Text].
Critelli G, Ferro G, Peschle C, Perticone FR, Rengo FR and Condorelli M (1977) Myocardial contractility after injection of prolonged infusion of magnesium sulphate. Acta Cardiol 32: 65-73[Medline].
Ekblom M, Hammarlund-Undenaes M and Paalzow L (1993) Modeling of tolerance development and rebound effect during different intravenous administrations of morphine to rats. J Pharmacol Exp Ther 266: 244-252[Abstract/Free Full Text].
Fawcett WJ, Haxby EJ and Male DA (1999) Magnesium: physiology and pharmacology. Br J Anaesth 83: 302-320[Abstract/Free Full Text].
Flatman PW (1991) Mechanisms of magnesium transport. Annu Rev Physiol 53: 259-271[Medline].
Foex P and Ryder WA (1979) Effect of CO₂ on the systemic and coronary circulations and on coronary sinus blood gas tensions. Bull Eur Physiopathol Respir 15: 625-638[Medline].
Friedman HS, Nguyen TN, Mokraoui AM, Barbour RL, Murakawa T and Altura BM (1987) Effects of magnesium chloride on the cardiovascular hemodynamics in the neurally intact dog. J Pharmacol Exp Ther 243: 126-130[Abstract/Free Full Text].
Hafen G, Laux-End R, Truttmann AC, Schibler A, McGuigan JA, Peheim E and Bianchetti MG (1996) Plasma ionized magnesium during acute hyperventilation in humans. Clin Sci Colch 91: 347-351[Medline].
Hampton EM, Whang DD and Whang R (1994) Intravenous magnesium therapy in acute myocardial infarction. Ann Pharmacother 28: 212-219[Abstract].
Huang YF, Upton RN and Runciman WB (1993a) IV bolus administration of subconvulsive doses of lignocaine to conscious sheep: relationships between myocardial pharmacokinetics and pharmacodynamics. Br J Anaesth 70: 556-561[Abstract/Free Full Text].
Huang YF, Upton RN and Runciman WB (1993b) IV bolus administration of subconvulsive doses of lignocaine to conscious sheep: myocardial pharmacokinetics. Br J Anaesth 70: 326-332[Abstract/Free Full Text].
Huang YF, Upton RN, Rutten AJ and Runciman WB (1992) IV bolus administration of subconvulsive doses of lignocaine to conscious sheep: effects on circulatory function. Br J Anaesth 69: 368-374[Abstract/Free Full Text].
Ising H, Bertschat F, Gunther T, Jeremias E and Jeremias A (1995) Measurement of free magnesium in blood, serum and plasma with an ion-sensitive electrode. Eur J Clin Chem Clin Biochem 33: 365-371[Medline].
James MF (1992) Clinical use of magnesium infusions in anesthesia. Anesth Analg 74: 129-136[Free Full Text].
James MF, Cork RC and Dennett JE (1987) Cardiovascular effects of magnesium sulphate in the baboon. Magnesium 6: 314-324[Medline].
Larrieu AJ, Newman GE, Syracuse DC, McClenathan JH, Gaudiani VA and Michaelis LL (1978) The effects of arterial CO₂ tension on regional myocardial and renal blood flow: an experimental study. J Surg Res 25: 312-318[Medline].
Makos JD, Malloy CR and Sherry AD (1998) Distribution of TmDOTP5- in rat tissues: TmDOTP5- vs. CoEDTA- as markers of extracellular tissue space. J Appl Physiol 85: 1800-1805[Abstract/Free Full Text].
Mandema JP and Wada DR (1995) Pharmacodynamic model for acute tolerance development to the electroencephalographic effects of alfentanil in the rat. J Pharmacol Exp Ther 275: 1185-1194[Abstract/Free Full Text].
Miller B, Craddock L, Hoffenberg S, Heinz S, Lefkowitz D, Callender ML, Battaglia C, Maines C and Masick D (1995) Pilot study of intravenous magnesium sulfate in refractory cardiac arrest: safety data and recommendations for future studies. Resuscitation 30: 3-14[Medline].
Murphy E, Freudenrich CC and Leiberman M (1991) Cellular magnesium and Na/Mg exchange in heart cells. Annu Rev Physiol 53: 273-287[Medline].
Nakaigawa Y, Akazawa S, Shimizu R, Ishii R, Ikeno S, Inoue S and Yamato R (1997) Effects of magnesium sulphate on the cardiovascular system, coronary circulation and myocardial metabolism in anaesthetized dogs. Br J Anaesth 79: 363-368[Abstract/Free Full Text].
Nattel S, Turmel N, Macleod R and Solymoss BC (1991) Actions of intravenous magnesium on ventricular arrhythmias caused by acute myocardial infarction. J Pharmacol Exp Ther 259: 939-946[Abstract/Free Full Text].
Raftos JE, Lew VL and Flatman PW (1999) Refinement and evaluation of a model of Mg²⁺ buffering in human red cells. Eur J Biochem 263: 635-645[Medline].
Runciman WB, Ilsley AH, Mather LE, Carapetis and Rao MM (1984) A sheep preparation for studying interactions between blood flow and drug disposition. Br J Anaesth 56: 1015-1027[Abstract/Free Full Text].
Runciman WB and Ludbrook GL (1993) Monitoring, in Anaesthesia 2nd ed. (Nimmo WS, Rowbotham DJ andSmith G eds) pp 704-739, Blackwell Scientific Publications, Oxford.
Scott JB, Frothlich ED, Hardin RA and Haddy FJ (1961) Na⁺, K⁺, Ca⁺⁺ and Mg⁺⁺ action on coronary vascular resistance in the dog heart. Am J Physiol 201: 1095-1100.
Stec GP and Atkinson AJ (1981) Analysis of the contributions of permeability and flow to intercompartmental clearance. J Pharmacokinet Biopharm 9: 167-180[Medline].
Upton RN (1996) A model of the first pass passage of drugs from i.v. injection site to the heart-parameter estimates for lignocaine in the sheep. Br J Anaesth 77: 764-772[Abstract/Free Full Text].
Upton RN, Huang YF, Mather LE and Doolette DJ (1999) The relationship between the myocardial kinetics of meperidine and its effect on myocardial contractility: model-independent analysis and optimal regional model. J Pharmacol Exp Ther 290: 694-701[Abstract/Free Full Text].
Upton RN, Huang YF, Grant C, Gray EC and Ludbrook GL (1996) Myocardial pharmacokinetics of thiopental in sheep after short-term administration: relationship to thiopental-induced reductions in myocardial contractility. J Pharm Sci 85: 863-867[Medline].
Upton RN, Ludbrook GL, Grant C and Doolette DJ (2000) The effect of altered cerebral blood flow on the cerebral kinetics of thiopental and propofol in sheep. Anesthesiology 93: 1085-1094[Medline].
van den Bos GC, Drake AJ and Noble MI (1979) The effect of carbon dioxide upon myocardial contractile performance, blood flow and oxygen consumption. J Physiol (Lond) 287: 149-161[Abstract/Free Full Text].
Zheng D, Upton RN and Doolette DJ (2000) In vivo manipulation and continuous measurement of muscle blood flow with venous effluent sampling. Clin Exp Pharmacol Physiol 27: 625-629[Medline].

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