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Cardiology Section, Department of Veterans Affairs Medical Center and Department of Medicine, University of Colorado Health Sciences Center, Denver, Colorado 80220
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ABSTRACT |
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 TOP
 ABSTRACT
 INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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Volume expansion and inotropic stimulation are used clinically to augment cardiac output during acute right ventricular (RV) pressure overload. We previously showed that a brief period of RV pressure overload causes RV free wall dysfunction that persists after normal loading conditions have been restored. However, the impact of volume expansion and inotropic stimulation on the severity of RV dysfunction after acute pressure overload is unknown. We hypothesized that the severity of RV dysfunction after RV pressure overload would be related to the level of RV free wall systolic stress during RV pressure overload, rather than to the specific interventions used to augment RV function. Chloralose-anesthetized, open-chest pigs were subjected to 1 h of RV pressure overload caused by pulmonary artery constriction, followed by 1 h of recovery after release of pulmonary artery constriction. A wide range of RV free wall systolic stress during RV pressure overload was achieved by either closing or opening the pericardium (to simulate volume expansion) and by administering or not administering dobutamine. The severity of RV free wall dysfunction 1 h after RV pressure overload was strongly and directly correlated with the values of two hemodynamic variables during RV pressure overload: RV free wall area at peak RV systolic pressure (determined by sonomicrometry) and peak RV systolic pressure, two of the major determinants of peak RV free wall systolic stress. Opening or closing the pericardium, and using or not using dobutamine during RV pressure overload, had no independent effects on the severity of RV dysfunction. The findings suggest that the goal of therapeutic intervention during RV pressure overload should be to achieve the required augmentation of cardiac output with the smallest possible increase in RV free wall systolic stress.
pressure-volume relation; mechanics; pericardium; dobutamine; pig
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INTRODUCTION |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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WHEN FACED WITH an acute increase in afterload, the normal right ventricle (RV) is able to increase peak systolic pressure to ~60 mmHg before RV contractile failure and systemic hypotension ensue. Increases in RV afterload are normally accompanied by reciprocal decreases in ejection fraction in a relationship similar to that which has been well described in the left ventricle (LV; see Ref. 2). It had been assumed that the decrease in RV ejection fraction observed during increased RV pressure was reversible and that restoration of normal loading conditions would be sufficient for complete normalization of RV contractile function. However, we have demonstrated that, under open-chest, open-pericardium conditions, increases in RV systolic pressure not severe enough to cause RV ischemia or systemic hypotension may nonetheless cause persistent RV systolic dysfunction that becomes apparent after restoration of normal loading conditions (5).
Interventions such as volume expansion and inotropic stimulation are used clinically to augment RV function during acute RV pressure overload. However, the impact of such interventions on the severity of RV dysfunction persisting after relief of RV pressure overload is unknown.
We hypothesized that the severity of RV dysfunction after RV pressure overload would depend on the level of systolic stress in the RV free wall during RV pressure overload rather than on the specific intervention used to augment RV function. To test this hypothesis, we subjected open-chest pigs to acute RV pressure overload while opening or closing the pericardium (to simulate volume expansion or contraction) and administering or not administering dobutamine to vary the relationship among RV systolic pressure, RV dilatation, and RV free wall stress.
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METHODS |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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This investigation conformed to the Guide for the Care and Use of Laboratory Animals published by the United States National Institutes of Health (NIH publication no. 85-23, revised 1985). It was approved by the Animal Studies Subcommittee of the San Francisco Department of Veterans Affairs Medical Center.
Experimental Preparation
The experimental preparation was similar to that reported previously (5). Twenty-eight female Yorkshire-Landrace pigs weighing 30-42 kg were anesthetized with ketamine hydrochloride (20 mg/kg im) and
-chloralose (100 mg/kg iv; Sigma Chemical, St. Louis, MO);
anesthesia was maintained with -chloralose (30-50
mg · kg
1 · h1
iv). The pigs were wrapped in a circulating warm water blanket to
prevent hypothermia. Normal saline solution was infused continuously at
150-250 ml/h iv. Pigs were intubated via tracheotomy and were ventilated with an air-O2 mixture using a pressure-cycled
ventilator adjusted to maintain PCO2 between 35 and 45 mmHg, pH between 7.35 and 7.45, and PO2
>100 mmHg.
After exposure via a midline sternotomy, the pericardium was opened,
and solid-state micromanometer catheters (Millar Instruments, Houston,
TX) were introduced into the RV via an internal jugular vein and into
the LV via a carotid artery (Fig. 1).
Bipolar pacing wires were affixed to the left atrial appendage. A
transit-time ultrasonic flow probe (Transonic Systems, Ithaca, NY) and
an umbilical tape snare were placed around the main pulmonary artery,
and a hydraulic occluder was placed around the inferior vena cava. Two orthogonal pairs of piezoelectric crystals were implanted in the mid-RV
free wall for determination of segment shortening using a
sonomicrometer (Triton Technology, San Diego, CA). The distance between
each crystal pair ranged from 1 to 1.5 cm. The crystals were aligned
parallel and transverse to the long axis of the RV outflow tract. An
intramyocardial electrogram was recorded from the crystal leads and was
used for timing of cardiac events. In experiments in which the
pericardium was reapproximated, a flat latex balloon connected to a
fluid-filled catheter was placed in the pericardial space to measure
intrapericardial pressure.
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Experimental Protocol
Autonomic blockade was produced with atropine (0.2 mg/kg iv) and either propranolol (1.0 mg/kg iv) in pigs not receiving dobutamine or hexamethonium (7.5 mg/kg iv) in pigs receiving dobutamine. The heart was paced ~10 beats/min faster than the spontaneous heart rate (except during dobutamine infusion).Baseline measurements of hemodynamics and RV function were made after verifying stability of the preparation for 30 min. The pulmonary artery was then gradually constricted over 15 min by using the umbilical tape snare to achieve the highest obtainable RV systolic pressure, while systemic arterial pressure was maintained near baseline by a titrated dose of phenylephrine (mean 175 µg/min iv). Pigs receiving dobutamine did not require or receive phenylephrine. After 1 h of pressure overload, the umbilical tape snare was released, and final measurements were obtained after a 1-h recovery period.
Four different conditions were employed during RV pressure overload
using a 2 × 2 factorial design as follows: in 13 pigs, the
pericardium was opened initially to permit instrumentation and baseline
measurements, reapproximated snugly and left closed during RV pressure
overload and the 1-h recovery period, and then reopened for final
measurements; in 15 pigs, the pericardium was left open throughout the
entire experiment; in 6 of the open pericardium and 6 of the closed
pericardium pigs, dobutamine (6 µg · kg1 · min1
iv) was infused during RV pressure overload. Measurements at baseline
and at 1 h of recovery were obtained with the pericardium open and
dobutamine off in all pigs.
Assessment of Regional and Global RV Function
Hemodynamic data were digitized at 200 Hz and recorded during brief suspensions of mechanical ventilation. To derive regional RV Frank-Starling relations under baseline and recovery conditions, three to six sets of data, spaced at intervals of at least 2 min, were recorded during 10-s occlusions of the inferior vena cava. Steady-state data (without inferior vena cava occlusion) were recorded under all three experimental conditions (baseline, RV pressure overload, and recovery).RV free wall area. RV free wall area was defined as the instantaneous product of the orthogonal crystal pair separations, i.e., the area subtended by the four sonomicrometry crystals. Sonomicrometry measurements depend in part on the intercrystal distance, a source of experimental rather than physiological variability. Therefore, sonomicrometry measurements were normalized to their baseline values in each pig.
RV free wall systolic area reduction. RV free wall systolic area reduction (a 2-dimensional analog to segment shortening in 1 dimension or ejection fraction in 3 dimensions) was defined as the difference between end-diastolic and end-systolic RV free wall area, divided by end-diastolic RV free wall area. End diastole was defined as the point corresponding to the peak of the R wave of the intramyocardial electrogram. End systole was defined as the point of maximum negative RV dP/dt.
Regional external work. Regional external work was defined as the area of an RV pressure-wall area loop (i.e., the 2-dimensional plot of RV pressure vs. RV free wall area) obtained during a single cardiac cycle.
To compare RV regional external work at recovery with the value determined at baseline under conditions of matched preload, RV regional Frank-Starling relations were used to calculate preload-adjusted regional external work (5). Briefly, the area of each RV free wall area-pressure loop obtained during a dynamic inferior vena cava occlusion (i.e., regional external work) was plotted against its corresponding end-diastolic RV free wall area, and the slope and intercept of the resulting Frank-Starling relation were determined by linear regression. RV regional external work was then calculated from the regional Frank-Starling relation slope and intercept in each pig, with preload (end-diastolic RV free wall area) set to its baseline, steady-state value. Figure 2 indicates how preload-adjusted regional external work is determined from regional Frank-Starling relations.
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Global RV stroke work. Global RV stroke work was defined as the integral of the instantaneous product of pulmonary artery flow (from the transit-time flow probe) and RV pressure over a single cardiac cycle.
Echocardiography. RV short axis echocardiographic views at the midwall were obtained using a GE RT6800 echocardiography system by placing a 5-MHz biplane transesophogeal echocardiography probe directly on the epicardial surface of the posterolateral LV free wall and imaging through the heart. Views were standardized by adjusting the image to obtain a circular LV cross section and imaging the RV just distal to the tips of the tricuspid valve leaflets during systole; this plane includes the area of RV free wall in which the sonomicrometry crystals were placed. Echocardiographic frames corresponding to peak RV systolic pressure (timed from the simultaneous electrocardiogram recording) were digitized and analyzed using NIH ObjectImage 1.62 software. For each cross-sectional view, points on the epicardial surface of the RV free wall at the anterior and posterior junctions with the interventricular septum and midway between these points were identified and used to calculate the short axis radius of curvature of the RV free wall.
Statistical Analysis
Measured hemodynamic variables at baseline, during pressure overload, and at recovery were compared using Student's t-test and the Bonferroni correction for multiple comparisons. Derived indexes of RV contractile function were normalized to baseline and tested for significance using one-sample t-tests. In addition, measured variables, including peak RV systolic pressure, RV end-diastolic pressure, end-diastolic RV free wall area, RV free wall area at peak RV systolic pressure, RV short axis radius of curvature, and dummy variables representing the presence or absence of inotropic stimulation or pericardial restraint during pressure overload, were entered into a forward stepwise linear regression model (F to enter = 4.000, F to remove = 3.996, where F is the F-test statistic). Those variables that predicted the severity of RV dysfunction at recovery (as measured by the fraction of baseline RV preload-adjusted regional external work) with P < 0.05 were considered to be significant. All data are reported as means ± SE.| |
RESULTS |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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Table 1 shows steady-state hemodynamic data
under each experimental condition for each of the four treatment
groups. Pulmonary artery constriction simultaneously increased peak RV
systolic pressure and decreased RV free wall systolic area reduction,
as anticipated. Pigs receiving dobutamine maintained somewhat higher RV
free wall systolic area reduction and cardiac output despite greater
peak RV systolic pressure compared with pigs not receiving dobutamine
during pressure overload. Opening the pericardium during RV pressure
overload permitted the RV to dilate and RV free wall area to expand
compared with baseline, especially in the absence of dobutamine.
Closing the pericardium during pressure overload limited both RV free
wall area at end diastole and RV free wall area at peak RV systolic
pressure to no more than their baseline values. The RV short axis
radius of curvature did not change significantly from baseline (2.5 ± 0.04 cm) to RV pressure overload (2.4 ± 0.04 cm) in any
group. At 1 h of recovery, RV systolic and diastolic pressures did not differ significantly from baseline, but RV free wall
systolic area reduction, global RV stroke work, and cardiac output were all depressed compared with baseline.
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Figure 2A shows representative RV pressure-wall area loops obtained by brief occlusion of the inferior vena cava under baseline conditions and at 1 h of recovery. Note that the loop areas, which are an index of regional external work, are smaller for any given end-diastolic RV free wall area at 1 h of recovery compared with baseline. Figure 2B shows the regional Frank-Starling relations derived from the data in Fig. 2A. The downward and rightward shift in the relation at 1 h of recovery compared with baseline indicates persistent contractile dysfunction of the RV free wall.
Table 2 summarizes the derived indexes of
systolic function at baseline and 1 h of recovery. (Inferior vena cava
occlusion was not performed, and regional Frank-Starling relations
therefore were not determined during pressure overload because these
relations are not linear, and therefore not interpretable, under these
conditions.) In the closed-pericardium/no-dobutamine group, there were
no significant changes from baseline to recovery in regional
Frank-Starling slope and intercept or preload-adjusted regional RV
external work; peak RV systolic pressure and RV free wall area during
RV pressure overload were lower in these pigs than in the other three
groups. In the other three groups, RV preload-adjusted regional
external work at 1 h of recovery was persistently and significantly
reduced compared with baseline even though peak RV systolic pressure
had returned to baseline. In these three groups, there were also trends to decreased regional Frank-Starling relation slope and increased intercept, consistent with a decline in contractility. Although these
changes were not all statistically significant, this may be because
neither one of these measurements alone is as sensitive to changes in
contractility as preload-adjusted regional external work, which
incorporates both of these variables.
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All variables measured during RV pressure overload were entered into a
stepwise multiple linear regression to determine the significant
predictors of RV dysfunction at recovery. Of the variables measured,
only RV free wall area at peak RV pressure and peak RV systolic
pressure during pressure overload were significant independent
predictors of the severity of RV dysfunction at recovery, with the
former a stronger predictor than the latter. These two variables
together accounted for 83% of the variability in the severity of RV
dysfunction (i.e., r2 = 0.83, P < .0001).
Note that closing or opening the pericardium and using or not using
dobutamine were not independent predictors of RV dysfunction at
recovery. Figure 3 shows the univariate
dependence of RV dysfunction after pressure overload on peak RV
systolic pressure (A) and RV free wall area at peak RV systolic
pressure (B) during RV pressure overload.
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To permit a graphical representation of the multivariate dependence of
RV dysfunction on peak RV systolic pressure and RV free wall area, we
used the above linear regression model to define a dysfunction
predictor index as
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![<IT>a</IT>[RVSP]<SUB>RVPO</SUB> + <IT>b</IT> <FR><NU>[RVWA]<SUB>RVPO</SUB></NU><DE>[RVWA]<SUB>baseline</SUB></DE></FR>](/content/vol278/issue5/fulltext/H1414/img002.gif)
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DISCUSSION |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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We found that the severity of RV dysfunction persisting at recovery after relief of RV pressure overload was closely related to two variables measured during RV pressure overload: RV free wall area at peak RV systolic pressure and peak RV systolic pressure. Neither pericardial restraint nor inotropic stimulation with dobutamine during RV pressure overload had independent effects on the severity of RV dysfunction after restoration of baseline loading conditions. Instead, pericardial restraint during RV pressure overload attenuated RV contractile dysfunction at recovery by reducing RV free wall area during pressure overload, whereas inotropic stimulation by dobutamine during RV pressure overload exerted a variable effect by increasing RV systolic pressure and decreasing RV free wall area at peak RV systolic pressure.
Because of the complex shape of the RV, wall stress cannot be
determined exactly. However, we can identify several variables that
affect wall stress and as a result would be anticipated to contribute
most significantly to RV dysfunction. First, according to the Laplace
relation, wall stress (
) in a thin-walled container is proportional
to the intracavitary pressure (P) and the local radius of curvature
(ROC) and is inversely proportional to the wall thickness (h)
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Only a few other investigators have studied changes in ventricular function consequent to acute volume or pressure overload. All of these prior studies were performed in the LV, and the results were not concordant. Pagliaro et al. (10) and Downing et al. (3) both reported that ventricular contractility declined after acute volume overload. The observed decline in contractility was transient in the former study but was persistent in the latter. However, in both of these studies, diastolic dilatation was severe (160% of baseline in the study by Downing et al. and >230% of baseline in the study by Pagliaro et al.). Lew (7) observed a transient increase in contractility after more modest volume loading in dogs (mean 12% increase in end-diastolic segment length). LeWinter et al. (8) also observed a transient increase in contractility in dogs subjected to simultaneous volume and pressure overload. In our study, diastolic dilatation was minimal, with mean diastolic RV free wall area during RV pressure overload unchanged from the baseline value. Our results in the RV may have differed from previous results in the LV because of a relatively greater increase in wall stress in the thin-walled RV.
This study was designed to elucidate hemodynamic factors that contribute to RV dysfunction after acute pressure overload. The potential cellular or structural mechanisms of persistent RV dysfunction after RV systolic pressure overload are uncertain. We previously showed that regional myocardial blood flow does not decrease and regional myocardial lactate release does not increase during RV pressure overload in this model, suggesting that ischemia was unlikely to explain the RV dysfunction (5). Alterations in excitation-contraction coupling or in the function of myocardial contractile proteins could have been induced by RV pressure overload. For example, acute pressure overload has been shown to activate mitogen-activated protein kinases in mouse hearts (6). Because such protein kinase activation is implicated in other conditions causing myocardial dysfunction (13), it is conceivable that it could lead to ventricular dysfunction in this model as well. Alternatively, it is possible that disruption of extracellular myocardial structural elements, such as collagen, or intracellular structural proteins could have occurred consequent to the elevated systolic wall stress. Alterations in both types of elements have been implicated in LV dysfunction in conditions such as ischemia and cardiomyopathy (1, 9, 14). Moreover, disruption of the extracellular collagen matrix has been demonstrated in isolated rat hearts subjected to elevated intracavitary pressure (4).
Limitations
Although both RV preload-adjusted regional external work and global stroke work were depressed after RV pressure overload, there was no significant relation between these two variables. This is not surprising, since global RV stroke work is dependent on global RV preload (end-diastolic volume) and interventricular interaction as well as intrinsic contractility of the RV free wall. We did not determine either global RV volume or the extent of interventricular interaction in this study; therefore, we could not adjust for these effects.Absolute quantification of wall stress in the RV free wall is extremely difficult with the use of currently available techniques because of heterogeneities in wall thickness and geometry. Moreover, because global function of the RV is a result of the combined contributions of the morphologically distinct conus and sinus regions (11) and the LV septum (12), a single global measurement of RV wall stress would not be physiologically meaningful. Instead, we measured several factors that contribute to wall stress over a small area of the RV free wall. We did not attempt to determine the radius of curvature in the RV long axis because of marked variability in the echocardiographic measurement. We therefore cannot exclude the possibility that incorporating an estimate of radius of curvature in the longitudinal direction would have affected our results. In addition, we chose a central portion of the RV free wall for our analysis; therefore, we cannot exclude the possibility that other regions of the RV behave differently. However, we did not identify differences in the response of the conus and sinus regions to acute RV pressure overload in a previous study (5).
Wall stress is most closely related to transmural RV pressure rather than to absolute intraventricular pressure. Therefore, we could have overestimated the effective transmural RV pressure in pigs undergoing pericardial restraint because of elevated intrapericardial pressure. In every experiment in which the pericardium was closed, we measured intrapericardial pressure with a flat, latex balloon attached to a fluid-filled catheter. Uncertainty in synchronizing the timing of measurements made with a fluid-filled system with those made with the intracavitary micromanometer made determination of instantaneous transmural RV pressure uncertain. However, when we repeated our analysis by subtracting either intrapericardial pressure at the time of peak RV systolic pressure or mean intrapericardial pressure from peak RV systolic pressure to obtain an estimate of RV transmural pressure, our findings were not significantly altered from the preceding analysis. Indeed, we had anticipated that pericardial restraint would have at most a small effect on effective peak RV systolic wall stress, because total cardiac volume within the pericardial space is diminishing at the time of peak RV systolic pressure.
It was not possible to determine directly from this study whether elevated RV free wall stress during acute RV pressure overload was a cause or merely a consequence of the RV free wall dysfunction, since RV free wall dysfunction might itself lead to RV systolic dilatation and hence to increased RV free wall area. However, peak RV systolic pressure and RV free wall area at the time of peak RV systolic pressure were more strongly correlated with the severity of RV dysfunction when those variables were measured at the beginning of the hour of RV pressure overload than when those values were measured at the end of the hour. Thus it seems more likely that elevated wall stress was the cause of subsequent dysfunction than vice versa.
Implications
Our findings show that, for any given RV systolic pressure, systolic RV dilatation during acute pressure overload significantly exacerbates RV contractile dysfunction that persists after recovery from acute pressure overload. In the management of patients with hemodynamic compromise due to acute pulmonary hypertension, consideration of these effects suggests a potential advantage to earlier use of inotropic therapy, compared with volume loading, when necessary to augment cardiac output.| |
ACKNOWLEDGEMENTS |
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This work was supported in part by National Heart, Lung, and Blood Institute Grants HL-3475 (to C. Greyson) and HL-49944 (to G. G. Schwartz) and by the Department of Veterans Affairs Medical Research Service (to G. G. Schwartz).
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FOOTNOTES |
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The costs of publication of this article were defrayed in part by the payment of page charges. The article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. §1734 solely to indicate this fact.
Address for reprint requests and other correspondence: C. Greyson, Cardiology (111B), Veterans Affairs Medical Center, 1055 Clermont St., Denver, CO 80220 (E-mail: Clifford.Greyson{at}UCHSC.edu).
Received 28 May 1999; accepted in final form 9 November 1999.
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REFERENCES |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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, Open pericardium, no
dobutamine; 
, open pericardium + dobutamine; 
, closed
pericardium, no dobutamine; 
, closed pericardium + dobutamine.
