Vol. 277, Issue 5, R1249-R1260, November 1999
INVITED REVIEW
Coronary flow regulation in the fetal sheep
Kent L.
Thornburg1,2 and
Mark D.
Reller2,3
Departments of 1 Physiology and
Pharmacology and Medicine (Cardiology) and
3 Pediatrics (Pediatric
Cardiology) and the 2 Congenital
Heart Research Center, Oregon Health Sciences University, Portland,
Oregon 97201
 |
ABSTRACT |
The two
ventricles of the fetal sheep heart have anatomic and biochemical
differences that account for their differing functional capabilities
and blood flows. Coronary flows to both ventricles have been measured
using radiolabeled microspheres [or left ventricular (LV) flow,
by Doppler sensor on the circumflex coronary artery] during
experiments of pressure loading and chronic and acute hypoxemia. Blood
flow to the left ventricle with its lower wall tension is about
two-thirds the flow per gram compared with the right ventricle (RV).
Acute systolic pressure loading of the RV to its maximal work
capability stimulates flow to double (from ~250 to 500 ml · min
1 · 100 g1), but to a level less
than stimulated by adenosine (750 ml · min1 · 100 g1). At all RV work
loads, LV flow remains at two-thirds RV flow. Resting myocardial flow
levels in fetuses that have been chronically hypoxemic are similar to
maximal adenosine-stimulated flows of normal fetal sheep. This flow
augmentation is evidently due to vascular remodeling because a normal
"flow reserve" of ~500
ml · min1 · 100 g1 during adenosine
administration remains. Acute hypoxemia stimulates myocardial flow to
extraordinary levels (>1.5
l · min1 · 100 g1), levels larger than can
be obtained with chemical dilation alone. LV flows do not exceed
adenosine-stimulated flows when nitric oxide synthase is antagonized.
We conclude 1) fetal RV coronary flow increases with RV work but to levels less than during adenosine stimulation; 2) the fetal heart is
designed to accommodate extremely high flows in response to acute
hypoxemia, partially through large production of nitric oxide; and
3) the fetal coronary tree is dramatically remodeled in response to chronic hypoxemia.
fetal heart; nitric oxide; adenosine; law of Laplace; fetal
hypoxemia; wall stress; heart ventricle; coronary
remodeling
| |
INTRODUCTION |
BEFORE DISCUSSING the regulation of blood flow to
immature myocardium, it may be helpful to recall the physiological
features that underlie fetal cardiac physiology. The technology to
study the chronically prepared fetal heart was not available until the 1970s. Therefore, many aspects of physiology of the normal fetal circulation were not determined until the 1970s and 1980s. Even now our
understanding of fetal cardiovascular physiology is primitive compared
with adult cardiovascular physiology. The fetal sheep heart has been studied, perhaps more than any immature mammal heart,
and, unless so indicated, the data presented herein come from the sheep
model during the last 15 days of gestation. There are undoubtedly
differences between the immature sheep and human hearts, but many of
the salient features that have been determined in sheep are known to be
applicable to the human heart as well as to other species.
| |
FETAL CIRCULATION |
The fetal circulation operates as two parallel circuits, differing from
the adult arrangement where pulmonary and systemic circuits are in
series (16). Therefore, by convention, the output of the fetal heart is
reported as the combined output of the two ventricles. As is the case
in the adult mammal, all of the upper body flow in the fetus is
returned to the right ventricle via the superior vena cava. However, a
substantial portion of the well-oxygenated inferior vena caval flow is
shunted away from the right ventricle and into the left ventricle
through the foramen ovale where it is distributed to the upper body
(21). Therefore, the heart and brain are assured of receiving
oxygen-rich blood. Blood flowing from the right ventricle has a low
oxygen saturation and output joins aortic flow via the ductus
arteriosus and perfuses lower body and placenta for reoxygenation (66).
| |
DIFFERENCES BETWEEN RIGHT AND LEFT VENTRICLES |
Throughout medical history the two fetal ventricles were viewed to be
anatomically identical. Dawes summarized the current thinking of 1968 (16)
The two sides of the foetal heart are of much the same shape and
size, like the twin kernels of a nut as Harvey put it, and thus very
different from the adult. So the right and left sides of the heart have
about the same capacity (as Pohlman showed in the foetal piglet, 1909;
58), are filled at approximately the same pressure, eject blood against
the same arterial pressure and so might reasonably be expected to have
about the same output.
It should not be surprising that investigators initially felt that
the ventricles were similar. Compared with the adult heart, where the
thin-walled right ventricle looks like an architectural afterthought
next to the dominant thick-walled left ventricle, the two ventricular
chambers and free walls of the fetal mammalian heart look relatively
similar. On closer look, however, substantial anatomic and cytological
differences between the two ventricles are evident and these carry
important physiological consequences.
Figure 1 shows examples of measurements of
right ventricle output as a fraction of the biventricular output in
early studies of the sheep heart. It was nearly 30 years ago that
Assali and colleagues (3) first showed that the right ventricle had a larger stroke volume than the left ventricle, whereas Dawes et al.
(17) had shown the opposite. Most experts now agree that the right ventricle ejects between 60 and 70% of the biventricular output in sheep with a lesser but clear-cut dominance in the human fetus as well (59).
View larger version (15K):
[in this window]
[in a new window]
|
Fig. 1.
Estimates of right ventricular flow as a percentage of biventricular
output in historical studies [Dawes et al., 1954 (17); Assali et
al., 1965 (3); Goodwin et al., 1966 (31); Heymann et al., 1973 (32);
Anderson et al., 1981 (1).]
|
|
We investigated the mechanism for right ventricular dominance by
measuring simultaneous outputs of the fetal ventricle using calibrated
electromagnetic flow sensors. It should be noted that the output
measured from the left ventricle could not include coronary flow
because the sensors were necessarily placed distal to the coronary
ostia. It was possible to change the filling pressures of the two
ventricles by adding and withdrawing blood and/or saline so that
simultaneous function curves could be constructed (30). The ventricular
function curve is one way of investigating the relationship between the
filling of the ventricle (preload) and the output of the ventricle
(10). Our function curves (Fig. 2) were not
"pure" because there were concomitant changes in arterial pressure during the generation of the curves and because it was difficult to get perfect transmural pressure measurements in
chronically prepared animals (75, 76). Nevertheless, these reproducible function curves were highly instructive. These experiments indicated that right ventricular stroke volume is greater than is the left because the right ventricle operates on a completely separate and
elevated function curve where the right stroke volume is higher at all
filling pressures (Fig. 2).
View larger version (12K):
[in this window]
[in a new window]
|
Fig. 2.
Average simultaneous function curves for all 12 fetuses were determined
by forcing average regression coefficients for ascending and plateau
limbs of right and left ventricular (RV and LV, respectively) function
curves through their respective average break-point stroke volume-mean
atrial pressure coordinates. RV function curve has a steep ascending
limb with a mean slope of 0.37 ± 0.17 ml · kg1 · Torr1
and a plateau limb with a mean slope of 0.01 ± 0.02 ml · kg1 · Torr1.
Stroke volume intercept of 2 limbs is 0.94 ± 0.19 ml · kg1 · min1.
LV function curve has a steep ascending limb with a mean slope of 0.36 ± 0.26 ml · kg1 · Torr1
and a plateau limb with a mean slope of 0.03 ± 0.02 ml · kg1 · Torr1.
Stroke volume intercept of 2 limbs is 0.63 ± 0.15 ml · kg1 · min1,
a value that significantly differs from intercept of right ventricular
stroke volume (P < 0.001).
[Borrowed with permission from Reller et al.
(65).].
|
|
To further investigate the elevation of the right ventricular function
curve, we made anatomic measurements of hearts that had been fixed at
their resting filling pressures. Table 1
shows that the right ventricular chamber is larger than the left
chamber as suggested by pressure-volume curves (55, 67). That is, the
right ventricular curve is always right-shifted compared with the left
(56) so that the right ventricular chamber contains more blood than the
left chamber at any given common filling pressure. With similar
ejection fractions, the larger right ventricle ejects up to 50% more
blood each beat.
The anatomic differences between the ventricles affect their function
in other ways. The law of Laplace predicts that the right ventricle
will have a higher resting wall stress due to its larger radius of
curvature-to-free wall thickness ratio (r/h, Table 1). Figure
3 shows the rapid decrease in fetal right
ventricular stroke volume with increasing pulmonary arterial pressure
compared with the left ventricle, which is hardly affected by the same increases in aortic pressure. This finding is important because it
demonstrates that the right ventricle is much less able to eject
against increasing arterial pressure than is the left. These data also
suggest that the fetal right ventricle performs more work than the left
and must meet more severe metabolic demands whenever fetal arterial
pressures are increased.
View larger version (15K):
[in this window]
[in a new window]
|
Fig. 3.
Simultaneous average stroke volumes of right and left ventricles in
response to increased arterial pressure for 9 fetuses. Stroke volume is
expressed as percent of control value and arterial pressure as
increment above control. Linear regression coefficient for each
ventricle was calculated, average slope forced through 100% on
y-axis, and lines extended through
pressure range studied. RV pressure sensitivity ( 2.5 ± 1.4%
stroke volume/Torr) was >5 times LV pressure sensitivity (0.5 ± 0.7% stroke volume/Torr; P < 0.001). [Borrowed with permission from Reller et al.
(65).]
|
|
The histological features of the ventricles also differ before birth to
serve their separate pump functions (46). The working myocytes of the
right ventricle are larger than those of the left, and the capillary
luminal area is greater (73). These differences between the ventricles
reverse after birth so that left ventricular myocytes become larger
than those on the right side (73) as left ventricular work load is
increased dramatically during postnatal life (72).
In summary, the right ventricle is different from the left, with a
larger chamber volume, a larger radius-to-wall thickness ratio, a
higher free wall stress, and greater sensitivity to increases in
arterial pressure. The right ventricle performs more work and has
higher metabolic requirements in the face of stresses when arterial
pressure is increased.
| |
REGULATION OF CORONARY FLOW |
Hemodynamics. The regulation of
coronary flow in adult myocardium has been studied extensively and
reviewed frequently (8, 22, 34, 38, 49). Intensive investigation of
coronary control has been driven by scientific curiosity and the
reality that coronary disease is the major cause of death in western
societies. However, our present state of knowledge is based almost
exclusively on study of mature myocardium. The fact that coronary
development may predispose adults for coronary disease (4) suggests
that further investigation of prenatal coronary physiology may be
important. The extent to which adult coronary findings apply to
embryonic and fetal myocardium must yet be determined.
The principal determinants of mean flow through any organ are driving
pressure and resistance to flow. In the heart, resistance to flow is
carefully regulated by integrating a number of interdependent factors
(22, 38), including tissue pressure, myocardial metabolism, myogenic
responses, neural and humoral stimulation, and flow-dependent shear
stress (53). Chilian and colleagues (38) have provided good evidence
that there are "microdomains" (vessels in different size
categories) that are regulated uniquely from neighboring domains. Thus
microvessels of one size may constrict under a stimulus that dilates
larger vessels and vice versa. The integration of all microdomains
under a given set of circumstances determines the actual resistance to
flow that becomes physiological reality.
The standard textbook explanation of flow as the ratio of driving
pressure (inflow minus outflow pressure) and resistance is useful for
understanding mean flow through a stationary hypothetical organ.
However, it is hard to imagine an organ being further from the
hypothetical than is the beating heart. For example, the driving pressure for the myocardium is difficult to define for any given portion of the cardiac cycle, because, although the inflow pressure to
the coronary tree is aortic pressure, the outflow pressure is not known
with certainty for any part of the cycle. Tissue pressure acts as a
powerful "surrounding pressure" during myocardial contraction,
making the outflow pressure moot for that moment. Tissue pressure is
also dependent on the degree of hydration of the extracellular
compartment. The driving pressure may be better defined as the
difference between aortic and diastolic pressure, where flow becomes
zero. In the adult, this may be as high as 40-50 mmHg (6).
Autoregulation. Increasing inflow
pressure to the coronary bed does not cause a proportional increase in
flow to working heart muscle. Instead, flow tends to stay constant over
a wide range of perfusion pressures through autoregulation (52). The
autoregulation term was defined by Johnson (1964) (37) as "the
intrinsic tendency of an organ to maintain constant blood flow despite
changes in arterial perfusion pressure." In adult dog,
autoregulation may be effective over a pressure range of some 70 mmHg
(33). The autoregulatory range for the fetal heart is unknown. The
mechanisms that underlie autoregulation in adult hearts are not known
with certainty. The autoregulatory response is thought to be mediated via locally produced metabolic factors that directly affect vascular smooth muscle, primarily vessels of <150 µm diameter (38). Although most investigators are convinced that tissue adenosine is very important as a regulator of vascular resistance in the heart, evidence
also points to other unidentified local regulators that may be crucial
participants in the autoregulatory mechanism (18). However, myogenic
responses (constriction stimulated by increased intralumenal pressure
and relaxation with decreased pressure) may also be simultaneously
invoked at all levels throughout the myocardium (38).
Matching flow to metabolic need. In
adult myocardium, coronary flow is closely linked to metabolic need. It
is well known that the total oxygen demand includes a requirement for
basal metabolic function and excitation-contraction coupling, as well as the potential energy in the myocardial wall after ejection. Changes
in factors that increase metabolic need such as wall stress, heart
rate, or contractility will stimulate increases in coronary flow
through resistance changes in the coronary bed (12, 19). In accordance
with the adenosine hypothesis, as proposed by Berne in 1963 (7),
adenosine is the key regulator of metabolically activated flow
alterations. In this model, adenosine is increasingly released as
working myocardial cells increase metabolic activity or as oxygen
becomes in short supply. Adenosine then diffuses among microcirculatory
elements, causing coronary vasodilation. Recent evidence indicates a
powerful relationship between interstitial adenosine concentration and
coronary flow (74). Thus adenosine could be the primary tissue
signaling molecule for matching flow to metabolic need. There are a
number of factors generated within the myocardium that alter coronary
resistance that are potential candidates for participating in the
autoregulatory mechanism. These include nitric oxide (NO; 23, 29),
endothelin (79), prostacyclin (23), atrial natriuretic factor (28),
bradykinin (23), and angiotensin II (29). Recent experiments showed
that cocaine administration to pregnant ewes causes dilation of the
fetal coronary bed without fetal hypoxemia (14, 56).
Coronary reserve. If the coronary bed
can be dilated to its maximum by an exogenous chemical agent, then the
difference between the resting coronary flow and the maximum can be
defined as the coronary vascular reserve (2, 11, 33). Figure
4 shows two theoretical pressure flow
curves in the adult dog, one at maximal chemical dilation
(curve
D) and one while the coronary bed is under autoregulatory control (curve
A). At any pressure, the difference between the A curve and the D curve is the flow reserve (e.g., R1 or
R2, Fig. 4). This figure illustrates
several points. 1) The calculated flow reserve value is
highly dependent on the perfusion pressure chosen for the measurement.
Thus a reserve value ranging from 0 ml/min at 25 mmHg perfusion
pressure to ~400 ml/min at 125 mmHg can be obtained in the same heart
preparation, depending on which pressure is chosen. The take-home
lesson is that the perfusion pressure must be defined for comparisons
between experimental conditions. 2)
A shift in either the A curve or the D curve will alter the calculated
value of flow reserve at any perfusion pressure, and, therefore, flow
reserve measurements must be interpreted in light of such possibilities
(34).
View larger version (14K):
[in this window]
[in a new window]
|
Fig. 4.
Diagram of pressure-flow relationships in normal left ventricle during
autoregulation (A) and maximal vasodilatation (D).
R1 and
R2 are coronary flow reserves at
mean coronary perfusing pressures of 75 and 100 mmHg when aortic
pressure and heart rate are constant. [Reproduced with permission
from Hoffman and Spann (34).]
|
|
Measuring coronary flow in the fetus.
Coronary flow is difficult to measure in the fetus because of the small
size of the fetal heart and because the heart is less accessible than
is the adult heart. In experimental animals, fetal coronary flow is
usually measured by the microsphere method as introduced by Rudolph and Heymann (69). This method takes advantage of the fact that small (15 µm) plastic spheres will distribute themselves in proportion to
tissue blood flow when injected and thoroughly mixed in the left
ventricle. Because the spheres are too large to traverse a capillary,
they are trapped in tissue in proportion to the flow to that tissue.
The number of spheres trapped in a portion of tissue can be quantified
by detecting a sphere label, such as radioactivity, color, or fluorescence.
Coronary flows in the fetal heart can also be studied by installing a
cuff-type Doppler sensor around the proximal left main coronary artery
or the circumflex coronary artery so that flow velocities can be
measured during changing experimental conditions (Fig.
5). The distribution of the circumflex
artery includes most of the left ventricular free wall and a small
portion of the septum. The output (Doppler shift) of the flow sensor
correlates nicely with flow measured by the microsphere method (63).
Figure 6 shows the flow-velocity profile of
the circumflex artery under resting conditions. The Doppler method
suffers from several liabilities. For a Doppler shift to correlate well
with flow, the diameter of the vessel must remain constant during the
measurement. Furthermore, the Doppler sensor only measures flow
velocities for the vessel that it surrounds so that right and left
ventricular flows cannot be compared unless a probe is placed on both
main coronary arteries. Doppler shifts must also be calibrated to yield
true flow. This is usually done by measuring a wide range of flows by
the microsphere method while recording the Doppler shift at each flow.
Once calibrated, the Doppler sensor allows continuous flow measurement.
Right ventricular myocardial flows are measured by the microsphere
method while left ventricular flows use both Doppler and microsphere
methods.
View larger version (27K):
[in this window]
[in a new window]
|
Fig. 5.
Diagrammatic representation of surgical preparation of fetal sheep for
evaluation of myocardial flow during incremental increases in pulmonary
arterial pressure and during adenosine infusion. A polyvinyl catheter
was placed in the pulmonary artery (PA) proximal to an electromagnetic
flow sensor (EMF) and an inflatable occluder (OCC). An ultrasonic
Doppler flow probe (DOP) was placed around left circumflex artery.
Catheters were also placed in carotid artery (CA), right atrium (RA),
left atrial appendage (LAP), and pericardial space (PC). Ao, aortic
isthmus; DA, ductus arteriosus; SVC, superior vena cava; LAD, left
anterior descending coronary artery. [Borrowed with permission
from Reller et al. (63).]
|
|
View larger version (13K):
[in this window]
[in a new window]
|
Fig. 6.
Circumflex coronary artery flow velocity (coronary Doppler output) and
flow from pulmonary arterial root as measured by electromagnetic
sensor. Note that flow to fetal myocardium is reduced significantly
during systole.
|
|
Myocardial oxygen consumption and coronary
flow. The list of determinants of myocardial oxygen
consumption is long and includes work load, heart rate, metabolic state
of the myocardium, and many other factors. The multifactorial nature of
oxygen consumption has made it an ongoing area of intense study in the
adult (12, 15, 20, 43, 68, 70). In contrast, few studies on oxygen consumption in the embryonic and fetal hearts have been reported.
Most of the foundational work for our understanding of fetal blood flow
and oxygen consumption was carried out during the previous decade by
Fisher et al. (24-26). They were the first to sample fetal
coronary sinus blood on a chronic basis and to measure changes in left
ventricular oxygen consumption, oxygen delivery, and substrate
utilization during the perinatal period and in adult life. The
significant finding of their work is that myocardial oxygen consumption
is similar in fetuses and adults (~9
ml · min1 · 100 g1) but with a striking
40% increase in the neonate when oxygen consumption is very high. They
also found that carbohydrate (lactate) accounts for a significant
portion of the myocardial fuel needs in the fetal sheep, whereas it
accounts for about one-third of the fuel needs of the adult heart, the
remainder being mostly lipid.
Because of its low partial pressure of oxygen, fetal arterial blood
carries about one-half the oxygen found in adult blood. Therefore one
might expect that coronary flow would be twice that found in the adult.
Fisher et al. (26) used the radiolabeled microsphere method to show
that, indeed, resting blood flow to the ventricles of the fetus is
roughly twice that of adult levels (Fig.
7). This figure also shows several other
features of myocardial flow during the life of an individual. First,
right ventricular flow is higher than left ventricular flow in the
fetus. This fits with the known differences in wall tension and work
load as mentioned above. Second, as work load dominance switches from
the fetal right ventricle to the left ventricle after birth, left
ventricular flow is increased and right flow decreases (72). Finally,
blood flow per unit heart tissue weight decreases from the newborn
period to adulthood. Fisher et al. (25) showed that left ventricular myocardial oxygen delivery is similar during the fetal period to levels
found in the adult but they found an increase in myocardial oxygen
delivery during neonatal life when left ventricular work loads and body
oxygen needs are especially high. On the other hand, right ventricular
oxygen delivery decreases from fetal levels throughout life (25).
Myocardial flow with right ventricular systolic
load. Figure 8 shows that
right ventricular stroke volume decreases with increasing pulmonary
arterial pressure as the proximal main pulmonary artery is acutely
constricted by an occluder. Stroke volume decreases as pulmonary
arterial pressure goes up until the heart generates a pressure where
the right ventricle fails to eject and stroke volume falls
precipitously (63). This sudden, reproducible drop in function at a
particular pressure, designated as the "toleration point," is a
feature of right ventricular function in the fetal sheep. Could oxygen
delivery be limiting the function of the right ventricle at the
toleration point? An acute increase in right ventricular pressure in
the adult circulation is associated with a significant coronary
vasodilatory response (27, 77). Would this be true for the fetus? The
flow limitation question was addressed by increasing systolic load in
increments between the resting pressure and the toleration point in
seven fetuses and measuring coronary flow by the microsphere method
(32) at each pressure increment. To check whether a maximal work load
would use all of the coronary flow reserve that could be theoretically
available to the ventricle, adenosine was infused into the left atrium
at a rate of 60 µg · min1 · kg1
(based on dose-response studies) to maximally dilate the coronary bed.
View larger version (14K):
[in this window]
[in a new window]
|
Fig. 8.
Plot of right ventricular stroke volume (ml/kg)-mean pulmonary arterial
pressure relation in a single fetus. Increases in pulmonary arterial
pressure were obtained by pulmonary occlusion. [Borrowed with
permission from Reller et al. (63).]
|
|
Figure 9 shows that right ventricular flow
increased as work load increased. This finding was expected (13, 34).
However, there were a number of unexpected findings from these studies. For example, left ventricular flow followed right ventricular flow as a
constant proportion, 0.65 ± 0.02 (SD), although loading conditions
for the left ventricle and coronary perfusion pressure did not change
significantly. The interdependence of coronary flow in the two
ventricles has not been studied in the fetus so that the mechanism of
left ventricular flow change with right ventricular loading remains a
mystery. However, the mechanical interaction between the ventricles has
been investigated in the newborn sheep (51). Also note that the maximal
flow that the ventricle could generate at the toleration point (Fig. 9,
P4) was significantly less than the flow obtained with chemical
dilation. It appears that the ventricle is not able to take advantage
of flow reserve even at the point where the ventricle is failing to
eject. This suggests, but does not prove, that oxygen delivery is not
the limiting factor causing the acute right ventricular failure in the
face of maximal systolic load.
View larger version (18K):
[in this window]
[in a new window]
|
Fig. 9.
Ventricular myocardial flow at 4 different pressure loads
(Control-P4) and during adenosine administration (Ad). Control had
a mean pulmonary arterial pressure of 53 mmHg, P2 is 57 mmHg, P3 is 63 mmHg, P4 is 71 mmHg. [Reproduced with permission from Reller et
al. (63).]
|
|
This study also showed that flow increased linearly with increases in
metabolic activity as judged by the product of heart rate and peak
systolic pressure (Fig. 10). This
so-called "double-product" or "rate-pressure product" is
commonly used as a quick estimate of changes in oxygen consumption for
the adult heart (45), although its use is approximate at best. It has
been shown that heart rate and pressure equally and independently
affect myocardial left ventricular oxygen consumption in the immature
heart as well (71) and that the rate-pressure products of the fetus and
adult are similar in magnitude (25). Unfortunately, it is not possible to sample venous blood draining the right ventricle to measure oxygen
uptake in that ventricle. Therefore testing the correlation of the
rate-pressure product and right ventricular oxygen consumption was not
possible in this study.
View larger version (18K):
[in this window]
[in a new window]
|
Fig. 10.
RV flow (±SD) as a function of heart rate-peak systolic blood
pressure product at 4 levels of systolic work load
(r = 0.98). [Reproduced with
permission from Reller et al. (63).]
|
|
In the adult heart there are regional variations in flow across the
free wall of the two chambers. In the mature left ventricle, subendocardial flow decreases more than subepicardial flow during ischemic episodes. Even though the free walls of the near-term fetal
heart are on the order of 4 mm in thickness (Table 1), it is possible
to separate the inner and outer layers of the myocardium to compare
flows (55, 56). Table 2 shows endocardial
to epicardial flow ratios with the increases in right ventricular
systolic pressure load. Note that no significant changes were found in
the ratio even with severe right ventricular systolic pressure loading.
Coronary flow with chronic fetal hypoxemia and
hypercapnia. To see whether chronic hypoxemia and
hypercapnia would alter coronary flow regulation, four near-term
fetuses that were too hypoxemic to be considered normal, were studied 7 days after surgery (64). In these fetuses, the carotid arterial blood
yielded a pH of 7.33 ± 0.01 (normal is 7.38),
PCO2 of 49.8 Torr (vs. 43 Torr), a
PO2 of 16.1 (vs. 20 Torr), and an
O2 content of 5.3 ml/dl (vs. 8 ml/dl). It was assumed that these fetuses had been hypoxemic since
surgery. When resting coronary flow was measured in these fetuses, it
was found that their resting flows were nearly identical to the maximal
flows obtained with adenosine in normoxemic animals (Fig.
11), even though their coronary perfusion
pressure was not changed (49.1 vs. normal 47.4 Torr). Therefore, it
appeared that the hypoxemia had exhausted the entire coronary flow
reserve. To test this hypothesis, adenosine was infused into the left
atrium as mentioned above. However, it was found that, surprisingly, a
flow reserve was present. Figure 11 shows that the flow reserve was
enormous and amounted to some 500 ml · min1 · 100 g1. The flows to the right
ventricle during adenosine infusion were astronomical, reaching well
over 1.0 l · min1 · 100 g1 during adenosine
infusion (with some individual flows over 1.5 l · min1 · 100 g1). Flows of this
magnitude are at least double maximal myocardial blood flow seen in the
adult myocardium under any circumstance (5, 44).
View larger version (19K):
[in this window]
[in a new window]
|
Fig. 11.
RV and LV myocardial blood flow using radiolabeled microsphere
technique. Myocardial flows were measured in normoxemic fetuses at
baseline (Control), during acute right ventricular pressure loading
(Load), and during adenosine administration (Adenosine;
n = 7; Ref. 12). Myocardial blood flow
was later measured in a group of chronically hypoxemic fetuses
(n = 4) at baseline (Control) and with
adenosine. Maximal myocardial flow with adenosine in hypoxemic fetuses
was significantly greater than any other measured flow. Baseline
(Control) hypoxemic myocardial blood flow was not different from
maximal myocardial blood flow in normoxemic fetuses. [Borrowed
with permission from Reller et al. (64).]
|
|
If adenosine is able to dilate the coronary to its chemical maximum,
the changes between normal and chronically hypoxemic hearts suggest a
substantial enlargement of the cross-sectional area at the level of
resistance vessels (33). This might indicate that the coronary tree has
remodeled to grow new resistance vessels or that resistance vessels
have grown to new diameters in the dilated condition, or both.
Regardless, these data suggest that the coronary vascular tree in the
immature heart is very plastic and able to remodel extensively to meet
the oxygen demands of the myocardium. Data from Vlahakes et al. (78)
indicate that loading conditions may also affect growth of resistance
vessels in the coronary tree of prenatal sheep but that this effect is lost after birth. In fetuses with anemia, the number of capillaries appears to increase with a concomitant increase in vascular endothelial growth factor (50). These findings fit with experiments in immature rabbits where chronic hypoxemia caused an increase in flow reserve (35,
36).
Left ventricular coronary flow with acute
hypoxemia. To what extent would coronary flow increase
if the fetus were to suddenly experience arterial hypoxemia? Would the
fetal heart then be able to use its entire chemical flow reserve, even
though it apparently could not do so when faced with a work load? If
the entire adenosine reserve is available, that would suggest that the
immature myocardium uses separate signaling mechanisms to augment
coronary flow to meet the demands of hypoxemia versus those of systolic
loading. These questions were addressed in a series of experiments
where 14 fetal hearts were equipped with a Doppler sensor on the
circumflex artery (see Fig. 5) so that flow velocity could be measured
during episodes of acute hypoxemia (62).
The experimental protocol included measuring control flows, flows
during adenosine administration, flows during fetal hypoxemia, flows
with the NO synthase inhibitor
N
-nitro-L-arginine
(L-NNA), and flows with both hypoxemia and
L-NNA. Fetuses were made acutely
hypoxemic by reducing the fraction of inspired oxygen to the ewe.
Average fetal arterial blood values during hypoxemia were pH 7.31 ± 0.06; PCO2 45.8 ± 9.3 Torr;
PO2 8.8 ± 0.8 Torr;
O2 content 1.7 ± 0.2 ml/dl. Table 3 shows the hemodynamic effects in
the fetus with these various treatments. It is important to note that
mean carotid pressure was increased during hypoxemic episodes and
during L-NNA administration.
View this table:
[in this window]
[in a new window]
|
Table 3.
Comparison of hemodynamic variables at baseline, during adenosine
infusion, with acute hypoxemia, with L-NNA infusion, and
with subsequent acute hypoxemia
|
|
During bouts of severe hypoxemia, the fetal coronary flows exceeded
chemical dilation with adenosine (Fig.
12, "Ad" vs. "Hypox"). At
first we thought this surprising result could be due to a
miscalculation of the dose so that the coronary tree was not fully
dilated by the dose of adenosine that we originally determined.
However, the maximal dilation by adenosine was the equivalent to that
found in previous experiments and, furthermore, increasing the dose even further did not bring about increases in flow. We then thought that the perfusion pressure might have increased enough to make the
reserve larger. From the pressure-flow curve generated during chemical
dilation, the small (5 mmHg) rise in arterial pressure could not
account for the powerful coronary dilation during hypoxemia.
View larger version (15K):
[in this window]
[in a new window]
|
Fig. 12.
Myocardial flow to left ventricle of sheep fetus. Note that flow is
higher with hyoxemia than during adenosine administration or with
hypoxemia plus N-nitro-L-arginine
(L-NNA) administration (H + LNN). Also note that flow was reduced with
L-NNA compared with control. All
flows are significantly different (* different from control;
** different from control and adenosine; P < 0.05)
except that Ad and H+LNN are not different. [Reproduced with
permission from Reller et al. (62).]
|
|
Next, in the same study we sought to determine the role of NO in the
normal control of coronary flow in the fetus and during arterial
hypoxemia. Blockade of NO synthase did reduce myocardial flow by some
30% at baseline (P < 0.05), with
the flow reduction becoming greater as oxygen content is reduced (Fig.
13; Ref. 57). Of great interest is the
fact that coronary flow did not exceed that during adenosine
administration when NO synthase was antagonized. These findings need to
be interpreted in light of recent data indicating that inhibiting NO
synthesis attenuates coronary dilation by adenosine (39). From this
investigation we learned the following. 1) NO production exerts a basal
coronary vasodilatory effect in the fetus, a finding that is
quantitatively similar to that seen in the adult circulation (42, 57).
2) The blockade of NO production by
the coronary endothelium had an unexpected effect on myocardial oxygen
consumption. This is shown in Fig. 14.
Although the rate-pressure product was not affected by adenosine or
L-NNA administration, nevertheless oxygen consumption was depressed by some 50% with the
blockade of NO synthase. This remains unexplained. A similar finding
was found by Bernstein et al. (9), but not by Maekawa et al. (48), in
adult dogs. 3) Acute hypoxemia in
the fetus induces a myocardial blood flow response that exceeds maximal flow obtained by adenosine at a similar perfusion pressure. This flow
response would appear to be unique to the fetus and to be at least in
part mediated by the NO pathway.
View larger version (15K):
[in this window]
[in a new window]
|
Fig. 13.
Relationship between coronary flow as assessed by left circumflex
coronary Doppler-flow velocities and arterial
O2 content in fetuses made
hypoxemic ( ) compared with similar degrees of hypoxemia during
L-NNA infusion ( ). Points on
2 curves were fitted using a 2nd-degree polynomial. Note that flow is
depressed at all oxygen contents when nitric oxide synthase is
antagonized. [Borrowed with permission from Reller et al.
(62).]
|
|
View larger version (15K):
[in this window]
[in a new window]
|
Fig. 14.
Myocardial oxygen consumption under 3 conditions. Note that
administration of adenosine did not affect oxygen uptake. However,
O2 consumption was reduced during
inhibition of nitric oxide synthase with
L-NNA. * Different from
baseline (P < 0.05). [Reproduced with permission
from Reller et al. (62).]
|
|
Yet these findings must be interpreted in light of elegant studies of
ewes kept at 3,820 m altitude during pregnancy. Kamitomoto et al. (40,
41) showed that fetuses raised at altitude had normal resting coronary
flows (~200
ml · min1 · kg1)
and increases in flow (~150%) similar to controls under acute hypoxemic stress conditions (fetal arterial
PO2 decreased acutely from 19 to 11 Torr). These studies point to our remaining ignorance regarding the
role of stage of development and duration of hypoxemia in generating a
coronary response in the fetus.
Regulation of atrial myocardial blood
flow. Hemodynamic data suggest that atrial function is
more important to ventricular filling in the fetus with a greater
contribution of atrial "systole" to ventricular end-diastolic
volume than for the adult (60). In addition, the fetus appears to rely
on a more coordinated atrial contraction to fill its less compliant
ventricles (55, 61, 67). Thus inadequate myocardial blood flow to the
fetal atria would likely compromise atrial and, therefore, ventricular
function. We postulated that atrial myocardial blood flow might be
compromised under conditions causing increased ventricular blood flow
and that this compromise could significantly alter atrial function and
ventricular filling in the fetus.
The fetal sheep that were placed in ventricular flow studies were also
evaluated to determine whether atrial myocardial blood flow is
regulated independently of fetal ventricular myocardial blood flow
(47). This investigation indicated several findings of interest. First,
at baseline, fetal atrial myocardial blood flows were less than half
that measured in the fetal ventricle per gram tissue (~90
ml · min1 · 100 g1 tissue for the right
atrium vs. 197 and 253 ml · min1 · 100 g1 for the left ventricle
and right ventricle, respectively). However, the crucial finding in
this investigation was that during acute pressure loading conditions,
the percent increase in atrial myocardial blood flow in response to
loading was actually greater than for ventricular myocardial blood flow
(a nearly 3-fold increase vs. a doubling of ventricular blood flow).
Furthermore, acute ventricular pressure loading was associated with
significant increases in right atrial a-wave pressure (active atrial
contraction), a finding that likely reflects an increase in atrial wall
stress and right atrial myocardial oxygen demand.
In summary, these findings indicate that atrial blood flow in the fetus
is regulated independently of ventricular myocardial blood flow and
that there is no evidence of any compromise of atrial blood flow with
increasing work load. Atrial flow actually exceeded ventricular flow.
Finally, the increase in right atrial systolic pressure with right
ventricular pressure loading suggests that atrial myocardial blood flow
regulation is influenced by atrial work.
| |
CONCLUSIONS |
Coronary reserve was found to be dependent on the experimental
conditions. We conclude that right ventricular flow is rapidly increased in response to increased systolic load, but we surmise that
the entire coronary flow reserve cannot be used in such circumstances. It also appears that right and left ventricular flows are linked even
if one ventricle is required to do all the work. We suspect that subtle
mechanical cross talk explains this phenomenon. Preliminary experiments
indicate that the coronary tree is highly plastic and responds to
conditions of chronic arterial hypoxemia by a substantial increase in
the cross-sectional area of the resistance portions of the coronary
tree. Coronary flows in hearts of fetuses that have been chronically
hypoxemic are enormous when the coronary bed is fully dilated. Acute
hypoxemia stimulates the normal fetal heart to dilate to levels that
exceed chemical dilation. This response is blocked by antagonism of NO synthase.
| |
THE FUTURE |
It is quite clear that the regulation of coronary flow in the immature
heart is so different from that of the adult that it warrants extensive
research. Several areas are particularly ripe for study.
1) Coronary flow appears to be
linked between the ventricles in unanesthetized fetuses. Further work
is required to confirm this finding. If such a link exists, the
mechanisms will prove to be important and fascinating.
2) The plasticity of the coronary tree before birth should be of interest to students of cardiac physiology, whether their interest is in the mature or immature myocardium. To what extent is the coronary tree in immature myocardium able to alter its growth? What are the chemical signals for remodeling the coronary tree? How are these chemical signals regulated and how is
their effectiveness altered with age of the individual? Is it possible
to regain plasticity in the aging heart?
3) The mechanisms that underlie the
regulation of coronary flow, on a moment-by-moment basis, have not been
studied. To what degree are these mechanisms similar to those of the
adult? Are there microdomains in the immature myocardium as postulated
for the adult coronary tree (39)? If so, how are they regulated and at
what stage of development do they arise?
4) Autoregulation has not been much
studied in the immature heart. Although it is clear that the coronary
reserve is large in the prenatal sheep heart, the shape and position of
the autoregulatory curve (if there is one) have not been described.
Figure 15 shows a hypothetical autoregulation curve and the genuine dilation pressure flow curve in
the sheep fetus (compare with Fig. 4).
5) The acute regulation of coronary
flow and the chronic regulation of coronary growth are under the
influence of a large number of genes that have not been studied during
development. How are these genes regulated and can they be manipulated
for therapeutic purposes?
View larger version (17K):
[in this window]
[in a new window]
|
Fig. 15.
Pressure-flow relationships of normal fetal heart.
Top line is fetal dilation curve
during adenosine administration, determined from experimental data (62)
with the adenosine point (A) at resting arterial pressure. H, flow
under hypoxemic conditions; W, under maximal working conditions; B,
under baseline conditions at rest. A hypothetical autoregulation curve
is drawn in to suggest a possible flow pressure relationship in fetus.
However, such a curve has not yet been constructed in fetus.
|
|
These questions are an intellectual gold mine awaiting those with pans,
sluice boxes, and a love of discovery.
| |
ACKNOWLEDGEMENTS |
The authors thank Drs. Mark Morton, George Giraud, C. Wright
Pinson, Jamie Lohr, David Wu, Mike Burson, Lowell Davis, and Antonio
Barbera for significant scientific contributions to these studies. The
authors also thank Linda Wolf, Lisa Rhuman, Zara Wanlass, and Emily
Gilster for friendship and clerical assistance. The authors thank
Jeanie and Kim for supporting their addiction to science.
| |
FOOTNOTES |
These studies were supported by the National Institutes of Health
Grants HL-43015 and HD-33430 and the Medical Research Foundation of Oregon.
Address for reprint requests and other correspondence: K. L. Thornburg,
Congenital Heart Research Center, L464, Dept. of Physiology & Pharmacology, Oregon Health Sciences Univ., Portland, OR 97201 (E-mail:
thornbur{at}ohsu.edu).
| |
REFERENCES |
1.
Anderson, D. F.,
J. M. Bissonnette,
J. J. Faber,
and
K. L. Thornburg.
Central shunt flows and pressures in the mature fetal lamb.
Am. J. Physiol.
241 (Heart Circ. Physiol. 10):
H60-H66,
1981.
2.
Archie, J. P.,
D. E. Fixler,
and
J. I. E. Hoffman.
Coronary reserve and right ventricular function in awake newborn lambs with persistent right ventricular hypertension.
Pediatr. Res.
11:
867-870,
1977[Medline].
3.
Assali, N. S.,
J. A. Morris,
and
R. Beck.
Cardiovascular hemodynamics in the fetal lamb before and after lung expansion.
Am. J. Physiol.
208:
122-129,
1965.
4.
Barker, D. J. P.,
A. R. Bull,
C. O. Osmond,
and
S. J. Simmonds.
Fetal and placental size and risk of hypertension in adult life.
Br. Med. J.
301:
259-262,
1990.
5.
Barnard, R. J.,
H. W. Duncan,
J. J. Livesay,
and
G. D. Buckberg.
Coronary vasodilator reserve and flow distribution during near maximal exercise in dogs.
J. Appl. Physiol.
43:
988-992,
1977[Free Full Text].
6.
Bellamy, R. F.
Calculation of coronary vascular resistance.
Cardiovasc. Res.
14:
261-269,
1980[Medline].
7.
Berne, R. M.
Cardiac nucleotides in hypoxemia: possible role in regulation of coronary blood flow.
Am. J. Physiol.
204:
317-322,
1963.
8.
Berne, R. M.
Regulation of coronary blood flow.
Physiol. Rev.
44:
1-29,
1964[Free Full Text].
9.
Bernstein, R.,
W. Shen,
X. Xu,
and
T. H. Hinze.
Nitro-L-arginine decreases myocardial oxygen consumption in response to isoproterenol infusion in awake dogs (Abstract).
Circulation
90, Suppl. I:
I-104,
1994.
10.
Bishop, V. S.,
H. L. Stone,
and
A. C. Guyton.
Cardiac function curves in conscious dogs.
Am. J. Physiol.
207:
677-682,
1964.
11.
Botham, M. J.,
J. H. Lemmer,
R. A. Gerren,
R. W. Long,
D. M. Behrendt,
and
K. P. Gallagher.
Coronary vasodilator reserve in young dogs with moderate right ventricular hypertrophy.
Ann. Thorac. Surg.
38:
101-107,
1984[Abstract].
12.
Braunwald, E.
Control of myocardial oxygen consumption.
Am. J. Cardiol.
27:
416-432,
1971[Medline].
13.
Braunwald, E.,
J. Ross, Jr.,
and
E. H. Sonnenblick.
Mechanisms of Contraction of the Normal and Failing Heart. Boston: Little Brown, 1976.
14.
Burchfield, D. J.,
A. Pena,
A. J. Peters,
R. M. Abrams,
and
D Philips.
Cocaine does not compromise cerebral or myocardial oxygen delivery in fetal sheep.
Reprod. Fertil. Dev.
8:
383-389,
1996[Medline].
15.
Coleman, H. N.,
E. H. Sonnenblick,
and
E. Braunwald.
Myocardial oxygen consumption associated with external work: the Fenn effect.
Am. J. Physiol.
217:
291-296,
1969.
16.
Dawes, G. S.
Foetal and Neonatal Physiology. Chicago: Year Book Medical, 1968.
17.
Dawes, G. S.,
J. C. Mott,
and
J. G. Widdicombe.
The foetal circulation in the lamb.
J. Physiol. (Lond.)
126:
563,
1954.
18.
Dole, W. P.,
N. Yamanda,
V. S. Bishop,
and
R. A. Olsson.
Role of adenosine in coronary flow regulation after reductions in perfusing pressure.
Circ. Res.
56:
517-524,
1985[Abstract/Free Full Text].
19.
Downy, J. M.
Myocardial contractile force as a function of coronary blood flow.
Am. J. Physiol.
230:
1-6,
1976.
20.
Elbeery, J. R.,
J. C. Lucke,
M. P. Feneley,
G. W. Maier,
C. H. Owen,
R. E. Lilly,
M. A. Savitt,
M. Hickey,
S. A. Gall,
J. W. Davis,
P. Vantrigt,
J. S. Rankin,
and
D. D. Glower.
Mechanical determinants of myocardial oxygen consumption in conscious dogs.
Am. J. Physiol.
269 (Heart Circ. Physiol. 38):
H609-H620,
1995[Abstract/Free Full Text].
21.
Faber, J. J.,
D. F. Anderson,
M. J. Morton,
C. M. Parks,
C. W. Pinson,
and
K. L. Thornburg.
Hemodynamics of shunts in the fetal lamb.
In: Cardiovascular Shunts: Alfred Benzon Symposium 21, edited by K. Johansen,
and W. W. Burggren. Copenhagen: Munksgaard, 1985.
22.
Feigl, E. O.
Coronary physiology.
Physiol. Rev.
63:
1-205,
1983[Abstract/Free Full Text].
23.
Fleming, I.,
J. Bauersachs,
and
R. Busse.
Paracrine functions of the coronary vascular endothelium.
Mol. Cell. Biochem.
157:
137-145,
1996[Medline].
24.
Fisher, D. J.,
M. A. Heymann,
and
A. M. Rudolph.
Myocardial oxygen and carbohydrate consumption in fetal lambs and in adult sheep.
Am. J. Physiol.
238 (Heart Circ. Physiol. 7):
H399-H405,
1980.
25.
Fisher, D. J.,
M. A. Heymann,
and
A. M. Rudolph.
Fetal myocardial oxygen and carbohydrate consumption during acutely induced hypoxemia.
Am. J. Physiol.
242 (Heart Circ. Physiol. 11):
H657-H661,
1982.
26.
Fisher, D. J.,
M. A. Heymann,
and
A. M. Rudolph.
Regional myocardial blood flow and oxygen delivery in fetal, newborn, and adult sheep.
Am. J. Physiol.
243 (Heart Circ. Physiol. 12):
H729-H731,
1982.
27.
Fixler, D. E.,
J. P. Archie,
D. J. Ullyot,
G. D. Buckberg,
and
J. I. E. Hoffman.
Effects of acute right ventricular systolic hypertension on regional myocardial blood flow in anesthetized dogs.
Am. Heart J.
85:
491-500,
1973[Medline].
28.
Focaccio, A.,
M. Volpe,
G. Ambrosio,
G. Lembo,
S. Pannain,
I. Enea,
S. Pignalosa,
and
M. Chiariello.
Angiotensin II directly stimulates release of atrial natriuretic factor in isolated rabbit hearts.
Circulation
87:
192-198,
1993[Abstract/Free Full Text].
29.
Gibbons, G. H.
Endothelial function as a determinant of vascular function and structure: a new therapeutic target.
Am. J. Cardiol.
79:
3-8,
1997[Medline].
30.
Gilbert, R. D.
Control of fetal cardiac output during changes in blood volume.
Am. J. Physiol.
238 (Heart Circ. Physiol. 7):
H80-H85,
1980.
31.
Goodwin, J. W.,
W. A. Mahon,
and
W. M. Paul.
Fetal cardiac output as studied by dye dilution techniques.
In: The Heart and Circulation in the Newborn and Infant, edited by D. E. Cassels. New York: Grune and Stratton, 1966.
32.
Heymann, M. A.,
R. K. Creasy,
and
A. M. Rudolph.
Quantitation of blood flow patterns in the foetal lamb in utero.
In: Foetal and Neonatal Physiology: Sir Joseph Barcroft Centenary Symposium. Cambridge: Cambridge University Press, 1973, p. 129-135.
33.
Hoffman, J. I. E.
Maximal coronary flow and the concept of coronary vascular reserve.
Circulation
70:
153-159,
1984[Free Full Text].
34.
Hoffman, J. I. E.,
and
A. E. Spann.
Pressure-flow relations in coronary circulation.
Physiol. Rev.
70:
331-390,
1990[Abstract/Free Full Text].
35.
Holmes, G.,
and
M. L. Epstein.
Chronic hypoxia increases coronary vascular reserve (Abstract).
Am. J. Cardiol.
66:
527A,
1990.
36.
Holmes, G.,
and
M. L. Epstein.
Effect of growth and maturation in a hypoxic environment on maximum coronary flow rates of isolated rabbit hearts.
Pediatr. Res.
33:
527-532,
1993[Medline].
37.
Johnson, P. C.
Review of previous studies and current theories of autoregulation.
Circ. Res.
15:
2-9,
1964.
38.
Jones, C. J. H.,
L. Kuo,
M. J. Davis,
and
W. M. Chilian.
Regulation of coronary blood flow: coordination of heterogeneous control mechanisms in vascular microdomains.
Cardiovasc. Res.
29:
585-596,
1995[Medline].
39.
Jones, C. J. H.,
L. Kuo,
M. J. Davis,
D. V. DeFily,
and
W. M. Chilian.
Role of nitric oxide in the coronary microvascular responses to adenosine and increased metabolic demand.
Circulation
91:
1807-1813,
1995[Abstract/Free Full Text].
40.
Kamitomoto, M.,
J. G. Alonso,
O. Takashi,
L. D. Longo,
and
R. D. Gilbert.
Effects of long-term, high altitude hypoxemia on ovine fetal cardiac output and blood flow distribution.
Am. J. Obstet. Gynecol.
169:
701-707,
1993[Medline].
41.
Kamitomoto, M.,
T. Ohtsuka,
and
R. D. Gilbert.
Effects of isoproterenol on the cardiovascular system of fetal sheep exposed to long-term high-altitude hypoxemia.
J. Appl. Physiol.
78:
1793-1799,
1995[Abstract/Free Full Text].
42.
Kelm, M.,
and
J. Schrader.
Control of coronary vascular tone by nitric oxide.
Circ. Res.
66:
1561-1575,
1990[Abstract/Free Full Text].
43.
Khalafbeigui, F.,
H. Suga,
and
K. Sagawa.
Left ventricular systolic pressure-volume area correlates with oxygen consumption.
Am. J. Physiol.
237 (Heart Circ. Physiol. 6):
H566-H569,
1979.
44.
Khouri, E. M.,
E. D. Gregg,
and
C. R. Rayford.
Effect of exercise on cardiac output, left coronary flow and myocardial metabolism in the unanesthetized dog.
Circ. Res.
17:
427-437,
1965[Abstract/Free Full Text].
45.
Kitamura, K. C.,
C. R. Jorgensen,
F. L. Gobel,
H. L. Taylor,
and
Y. Wang.
Hemodynamic correlates of myocardial oxygen consumption during upright exercise.
J. Appl. Physiol.
32:
516-522,
1972[Free Full Text].
46.
Legato, M.
Ultrastructural changes during normal growth in the dog and rat ventricular myofiber.
In: Developmental and Physiological Correlates of Cardiac Muscle, edited by M. Lieberman,
and T. Sano. New York: Raven, 1976.
47.
Lohr, J. L.,
M. D. Reller,
M. J. Morton,
D. E. Wu,
and
K. L. Thornburg.
Atrial myocardial blood flow during acute right ventricular pressure load and adenosine infusion in late gestation fetal sheep.
Pediatr. Res.
35:
325-328,
1994[Medline].
48.
Maekawa, K.,
D. Saito,
N. Obayashi,
S. Uchida,
and
S. Haraoka.
Role of endothelium-derived nitric oxide and adenosine in functional myocardial hyperemia.
Am. J. Physiol.
267 (Heart Circ. Physiol. 36):
H166-H173,
1994[Abstract/Free Full Text].
49.
Marcus, M. L.
The Coronary Circulation in Health and Disease. New York: McGraw-Hill, 1983, p. 65-92.
50.
Martin, C.,
A. Y. Yu,
B. H. Jiang,
L. Davis,
D. Kimberly,
A. R. Hohimer,
and
G. L. Semenza.
Cardiac hypertrophy in chronically anemic fetal sheep: increased vascularization is associtated with increased myocardial expression of vascular endothelial growth factor, and hypoxia-inducible factor-1.
Am. J. Obstet. Gynecol.
178:
527-534,
1998[Medline].
51.
Milstein, J. M.,
and
S. H. Bennett.
Increased right ventricular afterload alters left ventricular function in newborn lambs.
Am. Heart J.
114:
369-377,
1987[Medline].
52.
Mosher, P. J.,
P. A. Ross,
P. A. McFate,
and
R. F. Shaw.
Control of coronary blood flow by an autoregulatory mechanism.
Circ. Res.
14:
250-259,
1964[Abstract/Free Full Text].
53.
Muller, J. M.,
W. M. Chilian,
and
M. J. Davis.
Integrin signaling transduces shear stress-dependent vasodilation of coronary arterioles.
Circ. Res.
80:
320-326,
1997[Abstract/Free Full Text].
54.
Pena, A. E.,
D. J. Burchfield,
and
R. M. Abrams.
Myocardial and cerebral oxygen delivery are not adversely affected by cocaine administration to early-gestation fetal sheep.
Am. J. Obstet. Gynecol.
174:
1028-1032,
1996[Medline].
55.
Pinson, C. W.,
M. J. Morton,
and
K. L. Thornburg.
An anatomic basis for fetal right ventricular dominance and arterial pressure sensitivity.
J. Dev. Physiol. (Eynsham)
9:
253-269,
1987[Medline].
56.
Pinso
TOP
ABSTRACT
INTRODUCTION
