Vol. 277, Issue 5, H1924-H1930, November 1999
ACE inhibitors in HF restore canine pulmonary endothelial
function and ANG II
vasoconstriction
Ingrid M.
Straeter-Knowlen1,
Louis J.
Dell'italia1,3,
Jun
Dai2,
Gerald H.
Hankes4,
A. Raymond
Dillon4,
R. Earl
Cartee4,
Gerald M.
Pohost1, and
David D.
Ku2
1 Division of Cardiovascular
Disease, Department of Medicine and
2 Department of Pharmacology,
University of Alabama at Birmingham, Birmingham 35294;
3 Birmingham Veterans Affairs
Medical Center, Birmingham 35294; and
4 Auburn University College of
Veterinary Medicine, Auburn, Alabama 36849
 |
ABSTRACT |
Chronic mitral regurgitation (MR) in dogs
results in pulmonary congestion and increased cardiac
angiotensin-converting enzyme (ACE) activity and angiotensin (ANG) II
levels. ACE could contribute to altered pulmonary vasomotion in heart
failure, and ACE inhibitor (ACEI) therapy may normalize pulmonary
vasomotion. We evaluated pulmonary artery (PA) responses to ANG II and
bradykinin (BK) in control dogs, in dogs with 4 mo of MR, in MR dogs
treated with the ACEI ramipril (MR + R), and in control dogs treated
with ramipril (C + R). Mean PA systolic pressure increased in MR dogs
(21 ± 4 mmHg) but was normal in MR + R dogs (13 ± 1 mmHg).
Constriction of PA rings to ANG II was depressed in MR dogs. ACEI
treatment (MR + R) restored ANG II responsiveness, but peak ANG II
response (3.6 ± 0.2 g) in MR + R dogs remained lower than in C + R
dogs (4.7 ± 0.2 g). Endothelium-dependent relaxation to BK was
decreased (
87 ± 4% C, 65 ± 4% MR;
P < 0.05). Ramipril (MR + R) restored relaxation to BK. This demonstrates that pulmonary
congestion results in impaired pulmonary vasomotion to ANG II and BK,
which ACEIs could normalize, supporting the use of ACEIs in clinical management of chronic congestive heart failure.
ramipril; bradykinin; acetylcholine; pulmonary artery; mitral
regurgitation; heart failure; angiotensin-converting
enzyme
| |
INTRODUCTION |
CHRONIC HEART FAILURE LEADS to abnormalities in
vasomotor tone at rest, in response to vasodilatory stimuli, and during
exercise (11, 34, 35). It has been postulated that these abnormalities may result from changes in neural input, circulating and local hormonal
factors, and vessel wall structure (15). The renin-angiotensin system
(RAS), catecholamines, endothelin, vasopressin, and atrial natriuretic
factor have all been implicated in the altered regional and overall
cardiovascular function in heart failure. The influence of these
neurohormones has been described in large part in the systemic
peripheral vasculature. A direct effect of these traditional neurohormonal pathways on the development of pulmonary hypertension and
pulmonary vasoconstriction of congestive heart failure has not been
extensively studied. This could have important implications because
increased pulmonary vascular resistance can lead to right ventricular
functional impairment, which is a strong predictor of mortality in
heart failure (10, 24, 25, 27).
The Studies of Left Ventricular Dysfunction (SOLVD) and Survival and
Left Ventricular Enlargement (SAVE) demonstrated that chronic
angiotensin-converting enzyme (ACE) inhibitor (ACEI) therapy prevented
further deterioration in left ventricular function and decreased
coronary artery disease morbidity and mortality in patients with left
ventricular dysfunction without overt heart failure (26, 30). These
beneficial effects of ACEIs in asymptomatic patients suggest that
factors other than blood pressure reduction alone may be operating
under certain conditions (33). One such hypothesis is that ACEIs may
exert an important local effect on the RAS in both vascular and cardiac
tissues, whereas the circulating RAS remains normal in patients with
left ventricular dysfunction without overt heart failure (8, 14, 18).
However, there are few or no data regarding the beneficial effect of
chronic ACEI therapy in pulmonary vascular function.
Normal pulmonary vasomotor function, as in the other vascular beds,
depends on the delicate balance between the vasodilatory and
vasoconstrictory mechanisms. Increased ACE activity resulting in
increased degradation of bradykinin (BK) and increased ANG II could
contribute further to altered vasomotor function in heart failure. Thus
chronic ACEI therapy could provide two beneficial effects, decreased
ANG II formation and an increased preservation of BK. Pulmonary
vascular response to chronic ACEI therapy in an animal model of chronic
heart failure, however, has not been extensively evaluated (4).
We (7) have previously demonstrated that chronic volume overload
hypertrophy caused by mitral regurgitation (MR) in the dog results in
twofold increases in intracardiac ACE and chymase activity and
threefold increase in intracardiac ANG II peptide levels in the left
ventricle. This model is also characterized by increased pulmonary
pressures and increased circulating RAS components. We hypothesized
that heightened activity of the RAS in this model of heart failure
would result in abnormal vasomotor function in the pulmonary
vasculature and that these abnormalities could be reversed by chronic
ACEI therapy. Accordingly, we evaluated possible alterations in
vasoconstrictor responses to ANG II and endothelial cell (EC)-dependent
vasorelaxation to BK in intralobar pulmonary arteries from control
dogs, with and without chronic ACEI (ramipril) treatment, and from dogs
with chronic MR, with and without chronic ramipril treatment.
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METHODS |
Creation of MR and all follow-up care were performed at Auburn
University College of Veterinary Medicine. Four months after induction
of MR, animals were transported to the University of Alabama at
Birmingham Center for Nuclear Imaging Research in a fully equipped,
temperature-controlled van approved for this protocol. This study was
approved by the Institutional Animal Care and Use Committee at the
University of Alabama at Birmingham and by the Auburn University
College of Veterinary Medicine.
Percutaneous creation of MR.
Each dog was screened to rule out Ehrlichia canis et
platys and Dirofilaria
immitis before entering the protocol. To create MR,
each dog (18-25 kg) was anesthetized with intravenous Innovar-vet (droperidol and fentanyl 1-1.5 ml), intubated, and maintained on a
surgical plane of anesthesia with isoflurane (0.75-1.5%) and
oxygen (2 l/min). This anesthesia protocol was the same at the time of
percutaneous creation of MR and at the times of baseline and final
cinemagnetic imaging studies. The right carotid artery and jugular vein
were exposed through a sterile cutdown. A Swan-Ganz catheter (Baxter,
Deerfield, IL) was introduced into the jugular vein and advanced to the
pulmonary artery (PA) to record pulmonary artery pressure, pulmonary
capillary wedge pressure, and thermodilution cardiac output. A sheath
(8-Fr) was introduced into the carotid artery and placed into the left
ventricle under fluoroscopic guidance. A flexible, rat-tooth grasping
forceps (7-Fr; Cook Urological, Spencer, IN) was inserted into the
sheath and positioned at the mitral valvular apparatus where chordae
were cut to produce MR. Signs of significant MR included an increase in
the pulmonary arterial wedge pressure to >20 mmHg with V wave
dominance, a decrease in arterial pressure, and a decrease in cardiac
output of 50%. In addition, auscultation documented a new holosystolic
murmur and palpation of the precordium documented the presence of a
thrill in all dogs. When these hemodynamic and physical examination
criteria were accomplished, all catheters were removed, and the
surgical site was closed. The dogs were placed on antibiotics
(amoxicillin 20 mg/kg), and their hemodynamic status was closely
monitored for 24-36 h.
Follow-up care included daily monitoring of the heart rate, respiratory
rate, and temperature. The heart and the lungs were auscultated on a
daily basis. In each dog, serial chest radiographs were performed to
identify the onset of pulmonary venous congestion, and furosemide was
given at 2.2 mg/kg po bid if needed. Seven dogs were treated with
ramipril starting at 2.5 mg qid day and increasing to 10 mg bid at 1 wk. Three dogs started ramipril therapy at 24 h, and four
dogs started ramipril therapy at 3 wk after induction of MR. No
significant difference in cardiac hemodynamics and in isolated PA ring
studies between these two groups of ACEI-treated dogs was noted;
therefore, the results were combined and presented as MR + R. Four dogs
had MR and were untreated for 4 mo. All dogs were killed 4 mo after MR
was created. The control group consisted of eight dogs, and two of
these dogs were treated with the same amount of ramipril as the dogs in
the MR + R group.
Isolated intralobar PA ring preparations.
At the time of death, the dogs were anesthetized as described
previously, a left lateral thoracotomy was performed, and the heart was
KCl arrested. The left caudal lung lobe was harvested as quickly as
possible and immersed in ice-cold Krebs-Henseleit (KH) solution. The
intralobar PA was then identified in the left caudal lung lobe,
isolated, and cleaned of surrounding tissues in prewarmed (37°C)
and oxygenated (95% O2-5%
CO2) KH solution containing (in
mM) 118 NaCl, 4.6 KCl, 27.2 NaHCO3, 1.2 MgSO4, 1.2 KH2PO4,
1.75 CaCl2, 0.03 Na2EDTA, and 11.1 glucose as
previously described (16). Each vessel was cut into rings 5-mm long and mounted by means of two L-shaped 27-gauge stainless steel needles and
placed in 10- or 5-ml jacketed chambers containing prewarmed and
oxygenated KH solution. The upper needle was attached to a force-displacement transducer (Grass FT.03C) by a silk suture. The
vessels were passively stretched to 2 g for isometric force recording on a
Grass polygraph (model 7C). After 40 min of equilibration, the vessel
rings were exposed to two successive dosages of maximum depolarizing
KCl (80 mM). When contractile responses plateaued, the vessel rings
were rinsed with KH and allowed to equilibrate for 1 h with 5 µM
indomethacin before start of the experiment. It has previously been
shown (17) that this concentration of indomethacin results in complete
inhibition of cyclooxygenase and production of prostanoids.
Pretreatment with indomethacin will block the EC-dependent
cyclooxygenase-derived contribution to vasodilation (i.e.,
prostacyclin). All drug concentrations given are the final
concentrations as they appear in the tissue baths.
For endothelium-dependent relaxation, data are expressed as percentages
of relaxation or percentages of decrease in phenylephrine (PE)-induced
constriction. BK or ACh was added in cumulative fashion to the bath to
establish dose-response curves as soon as tension had stabilized. To
document the role of endothelium and nitric oxide on the observed
relaxation, studies were repeated in separate series of pulmonary
arteries with disrupted endothelium by mechanical abrading of the lumen
of each vessel with a wooden applicator and pretreatment of the vessels
with a specific nitric oxide synthase inhibitor,
NG-monomethyl-L-arginine
(L-NMMA, 0.25 mM) before BK and
ACh testing. For the contraction studies, cumulative dose
responses to ANG II and phenylephrine were performed in all
endothelium-disrupted pulmonary arteries. The vasoconstrictor effects
of each drug tested were normalized by expressing the data as a
percentage of the maximum constriction induced by KCl (80 mM) in the
same vessel ring.
Drugs and chemicals.
ACh, ANG, BK, indomethacin, phenylephrine, and sodium nitroprusside
were purchased from Sigma Chemical (St. Louis, MO).
L-NMMA was purchased from
Calbiochem, (La Jolla, CA). Losartan was kindly provided by Merck
Pharmaceutical. All drug solutions were prepared just before use.
Laboratory reagents and chemicals used for the preparation of KH
solution were purchased from Fisher Chemical (Pittsburgh, PA).
Plasma ANG II peptide levels.
Cardiac ANG peptide concentrations were determined by a method recently
described from our laboratory that combines solid-phase extraction
(SPE), HPLC, and RIA (20). AG50WX4 (200-400 mesh) cation exchange
resin was used in an SPE procedure for sample purification. The
recovery from the SPE procedure has been previously determined in our
laboratory using both labeled and unlabeled ANG peptides (21). With the
use of 125I-labeled ANG I (1.4 × 107 counts/min) and
125I-labeled ANG II (9 × 106 counts/min), recoveries were
93 ± 2% (n = 6) and 91 ± 2%
(n = 6), respectively. With the use of
0.5, 1.0, or 1.5 mmol of unlabeled ANG I and II, recoveries were 91 ± 9% (n = 6) and 90 ± 1% (n = 6), respectively (20).
Separation was performed by reversed-phase HPLC on a phenyl silica gel
column with an eluent consisting of 20% acetonitrile in 0.1 M ammonium
phosphate buffer (pH = 4.9). Aliquots (100 ml) of each relevant
fraction of column effluent were subjected to RIA immediately on
collection. Elution of standard ANG peptides under isocratic conditions
revealed clear resolution of ANG I, II, and III and ANG-(1-7) and
ANG-(3-8) peptides. RIA of relevant peaks revealed detectable
levels of ANG I and II in all heart tissues examined. Antibodies to ANG
I and II were raised in our laboratory in New Zealand White rabbits
immunized against peptides conjugated to
poly-L-lysine, as previously
described (20). The cross-reactivity of anti-ANG I antiserum with ANG II and of anti-ANG II antiserum with ANG I was <0.5%. The
sensitivity of the RIA for ANG I was 4 pg/ml and for ANG II was 2 pg/ml.
Statistical analysis.
All values are reported and graphed as means ± SE. Different PA
ring preparations (2-5) were studied from each dog for each of the
experimental protocols. The data for the control and the C + R group
were pooled because there was no statistically significant difference
between these groups. For the determinations of
IC50 and half-maximal effective
dose (ED50) values, the 50%
values of the log dose-response curves were used. The data were
analyzed statistically using ANOVA for repeated measures followed by
the Student's unpaired t-test.
P < 0.05 was considered
statistically significant.
| |
RESULTS |
Hemodynamics.
Four months after induction of MR, pulmonary arterial (21 ± 3.5 mmHg) and pulmonary capillary wedge (15 ± 2.2 mmHg) pressures increased significantly in the MR dogs compared with the control values
(13.3 ± 1.4 and 9.2 ± 1.4 mmHg, respectively). However, in the
ramipril-treated MR dogs, at the end of the 4-mo period, no significant
change in the pulmonary arterial (13 ± 1.0 mmHg) and pulmonary
capillary wedge (9 ± 0.6 mmHg) pressures were noted. These data
demonstrate the presence of pulmonary congestion and related heart
failure in our experimentally induced MR dogs. Chronic treatment with
the ACEI ramipril was effective in reversing these hemodynamic changes.
Clinically, there were no significant differences between the groups,
including necessity of treatment with furosemide.
Vasoconstrictor responses of PA rings.
Addition of ANG II (0.1-10 nM) produced a potent dose-dependent
contraction in isolated intralobar pulmonary arteries of control dogs,
reaching a maximum of 4.7 ± 0.2 g and
ED50 of log 9 (Table 1). Figure
1A
shows the actual contractile tension developed in response to
increasing concentrations of ANG II in control, MR, and MR + R dogs.
Figure 1B shows the same results after
they were normalized as a percentage of maximum KCl contraction in each
vessel ring. Chronic pulmonary congestion and heart failure in MR dogs
resulted in a significant shift of the dose-response curve to the right
and decreased both sensitivity
(ED50 of log 8.5) and
extent of maximum contractile response (3.5 ± 0.4 g) to ANG II.
Treatment of control dogs with ramipril did not alter the ANG II
constrictor response (data not shown), whereas similar ramipril
treatment in the MR dogs completely restored the sensitivity of the
pulmonary arteries to ANG II constrictor response. The maximum
contractile response of the MR + R dogs, however, remained significantly lower (3.6 ± 0.2 g) than in the control dogs (Table 1, Fig. 1). The dissociation constants
(KB)
of ANG II-induced contraction, determined in a subset of control and MR
dogs in the presence of the specific ANG II receptor
(AT1) blocker losartan (10 nM),
were not significantly different between the control (KB = 14 nM) and the MR
(KB = 9.5 nM)
dogs (Fig. 2). These results indicate that
the decreased response to ANG II in MR dogs was probably related to a
downregulation of the AT1
receptors and not caused by AT1
receptor dysfunction in the MR dogs with chronic congestive heart
failure.
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Table 1.
Effects of MR and ACEI treatment on ANG II-induced vasoconstriction
on isolated, endothelium-denuded canine pulmonary arteries
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Fig. 1.
Concentration-response relationships of ANG II-induced contraction in
isolated, endothelium-denuded intralobar pulmonary arteries of control
( ), mitral regurgitation (MR;  ), and MR and ramipril-treated (MR + R;  ) dogs. A: actual contractile
tension developed following cumulative addition of ANG II (0.1-10
nM). B: same data when contractile
responses were expressed as percentage of maximum contraction observed
in 80 mM KCl in same vessel rings. Data points represents means
(control, 18 rings; MR, 18 rings; MR + R, 22 rings); vertical lines
indicate ±SE. * Statistical difference from control at
P < 0.05.
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Fig. 2.
Effects of losartan on ANG II-induced contraction in isolated,
endothelium-denuded pulmonary arteries in control ( ; A)
and MR (; B) dogs. Losartan (0.01 and 0.1 µM; and
 , respectively) was added to tissue bath 20 min before ANG II
testing. Each point represents mean (control, 2 dogs, 4 rings; MR, 2 dogs, 4 rings); vertical lines indicate ±SE.
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To further investigate the mechanism(s) of altered ANG II response in
the MR dogs, dose-dependent contractile responses to 
-adrenergic
receptor activation by phenylephrine were also evaluated. Figure
3 shows that the dose-response curves to
phenylephrine-induced contraction were not significantly different
among the control, MR, and MR + R pulmonary arteries, suggesting that
the changes in ANG II responses in MR dogs were probably ANG II
receptor specific and not a generalized vascular smooth muscle cell
contractile dysfunction.
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Fig. 3.
Concentration-response relationships of cumulative addition of
phenylephrine (0.01-0.3 µM) in isolated, endothelium-denuded
pulmonary arteries in control (), MR (), and MR + R () dogs.
Each point represents mean (control, 15 rings; MR, 16 rings; MR + R, 18 rings); vertical lines indicate ±SE.
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Relaxation response of PA rings.
In all phenylephrine-precontracted and indomethacin-pretreated control
pulmonary arteries, cumulative addition of 0.1 nM to 0.1 µM of BK
resulted in a dose- and endothelium-dependent relaxation reaching a
maximum of 87 ± 4%. Mechanical disruption of intimal endothelium and pretreatment with the specific inhibitor of nitric oxide synthase, 0.25 mM L-NMMA,
completely abolished the observed BK relaxation (data not shown).
Induction of chronic congestive heart failure with MR in MR dogs
resulted in a significant depression of the BK-induced
endothelium-dependent relaxation. As shown in Fig.
4,
IC50 of BK-induced relaxation was
increased from 9 to 90 nM, respectively, in the control and the MR
dogs. Similarly, the maximum relaxation to 0.3 µM BK was
significantly reduced to 66 ± 4% in the MR dogs. However,
chronic treatment of the MR dogs with the ACEI ramipril completely
restored the BK relaxation response (Fig. 4).
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Fig. 4.
Concentration-response relationships of bradykinin (BK)-induced
endothelium-dependent relaxation of isolated pulmonary arteries of
control (), MR (), and MR + R () dogs. Relaxation after
cumulative addition of BK (0.1-0.3 µM) was expressed as
percentage of decrease in phenylephrine-induced constriction. Each
point represents mean (control, 15 rings; MR, 18 rings; MR + R, 24 rings), vertical lines indicate ±SE. * Statistical difference
from control at P < 0.05.
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As shown in Fig. 5, similar alterations in
ACh-induced, endothelium-dependent relaxation in the MR dogs and their
restoration when treated with ramipril were also observed. Maximum
relaxation response to 3 µM ACh was decreased from 88 ± 3% (control dogs) to 75 ± 5% (MR dogs). The maximum ACh
relaxation in the ramipril-treated MR dogs was 83 ± 4%,
which was not significantly different from the control.
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Fig. 5.
Concentration-response relationships of ACh-induced
endothelium-dependent relaxation in isolated pulmonary arteries of
control (), MR (), and MR + R () dogs. Relaxation following
cumulative addition of ACh (0.001-3 µM) was expressed as
percentage of decrease in phenylephrine-induced constriction. Each
point represents mean (control, 12 rings; MR, 20 rings; MR + R, 18 rings); vertical lines indicate ±SE. * Statistical difference
from control at P < 0.05.
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Circulating ANG II peptide levels.
Plasma ANG II peptide levels were significantly elevated in a subset of
MR dogs compared with control dogs (28 ± 27 pg/nl in control,
n = 2, vs. 435 ± 299 pg/nl in MR
dogs, n = 3) (Fig. 6). Treatment of MR dogs with the ACEI
ramipril prevented the increases in circulating ANG II peptide levels
(78 ± 34 pg/nl; n = 3).
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Fig. 6.
ANG II plasma levels in control, MR, and MR + R dogs. Values are
expressed as means ± SE. * Statistical difference from
control at P < 0.05;
** statistical difference from MR dogs.
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| |
DISCUSSION |
We previously reported that percutaneous chordal rupture of the mitral
valve in dogs resulted in pulmonary venous congestion and volume
overload-induced left ventricular heart failure (7). More importantly,
we reported that myocardial hypertrophy associated with this
pathological state was accompanied by marked increases in cardiac ACE
activity and tissue ANG II levels (7). Results of the present study
confirmed these findings and further demonstrated that initiation of
ACEI therapy, either early (24 h after the surgical mitral valve
chordal rupture) or late (3 wk after induction of MR), prevented the
associated pulmonary congestion and hypertension in these dogs with
mitral valve insufficiency. A significant decrease in plasma ANG II
levels was also observed in the animals treated with the ACEI ramipril
compared with MR dogs not treated with the ACEI. These findings suggest
a close relationship between the elevation of ANG II levels and the
volume overload induced congestive heart failure. Thus the present
animal model of congestive heart failure caused by chronic MR provides
a useful tool for the investigation of the role of ANG II in the
regulation of cardiovascular function.
ANG II is one of the most potent vasoconstrictors known and has also
been implicated in the development of various pathophysiological hypertensive diseases (9, 13). In addition to the direct action on
vasomotion, ANG II has also been shown to induce marked structural
changes in the vasculature, and the resulting vascular hypertrophy and
remodeling may enhance vasoconstriction and sustain hypertension (9).
Indeed, a similar role of ANG II in the regulation of pulmonary
vascular function and its associated increases during the development
of pulmonary hypertension have been reported (4, 24). Accordingly, it
is presumed that ANG II mediates a potent vasoconstrictor response in
the systemic and pulmonary vasculature in vivo.
Our in vitro studies demonstrate a significant decrease in the
contractile response and sensitivity to ANG II in the PA of MR dogs,
whereas the -adrenergic receptor-mediated contraction was not
altered in the same pulmonary vessels. This suggests a specific and
selective perturbation of ANG II receptor function in the lungs of dogs
with MR-induced heart failure. The marked elevated plasma ANG II levels
in our MR dogs could have mediated a compensatory decrease in ANG II
receptor function, possibly via an alteration in the specific signal
transduction pathways, thereby accounting for the decreased ANG II
constrictor response. Indeed, Cheng and co-workers (5) demonstrated a
decreased contractility response to ANG II in isolated cardiocytes from
dogs with chronic heart failure caused by rapid pacing. Alternatively,
it is possible that a specific downregulation of
AT1 receptor numbers could occur during chronic MR. This is substantiated by receptor binding studies in
numerous other animal models of hypertrophy and heart failure, which
demonstrated that AT1-receptor
density in the heart and kidney was significantly reduced after ANG II
infusion in the rat in vivo (29). Recently, heart failure in human
patients resulted in a selective downregulation of the
AT1 receptor (6, 31). Because ANG
II is known to be one of the most potent factors in the regulation of
gene expression of RAS components, it could account for the altered ANG
II receptor function observed in the pulmonary vasculature. However, to
our best knowledge, this present study is the first study to describe
decreased functional response to ANG II in PA vessels in heart failure.
However, one study (28) in the literature found that arterial
vasoconstrictor response to ANG II is enhanced in pacing-induced heart
failure in the dog. Another study demonstrated that canine lung lobes
after pacing-induced heart failure and pulmonary hypertension show
enhanced arterial vasoconstriction induced by norepinephrine after
-blockade (32). The reason for the difference between their data and
ours may be that in the lung lobes, changes in vascular tone are
dominated by those in resistance microvessels rather than the larger
conduit vessels studied in our dogs. Also, results from the present
paper are obtained under isometric conditions, whereas those in lung lobes are under isotonic conditions, which can lead to differences in
sensitivity (3). Furthermore, there could be model-specific changes in
pulmonary vascular function, i.e., pacing versus MR.
Our finding that chronic treatment with an ACEI such as ramipril is
able to reverse and normalize the sensitivity of the PA to ANG II
further supports our contention that adaptation of ANG II receptor
function and/or density may have occurred. However, it is interesting
to note that although the sensitivity of ANG II response was recovered,
the peak ANG II response in the MR + R dogs remained decreased compared
with the control dogs. The potential role of this complex
interaction in mediating the response of pulmonary pressures in vivo
requires further investigation.
Another important finding of this study was the significantly decreased
EC-dependent relaxation of the pulmonary arteries of MR dogs in
response to both BK and ACh. Bradykinin exerts its effects on the
endothelium through BK2 receptors
by activating endothelial nitric oxide synthase and also by activating
arachidonic acid conversion to prostacyclin. ACh is a choline ester
that exerts a vasodilatory response of most vascular beds through
muscarinic receptors located on the endothelial cells with subsequent
release of endothelium-derived relaxing factor (EDRF) (1, 2, 12, 22).
Thus the decrease in the vasodilatory response to BK and ACh in the
pulmonary arteries of MR dogs suggests a generalized endothelial
dysfunction in this vascular bed rather than a BK-specific alteration
in the endothelium-mediated relaxation. Such a generalized endothelial
dysfunction could be caused by a diminished EDRF (nitric oxide)
production and/or release in the MR pulmonary arteries. Similar findings have been reported with endothelial cell dysfunction during heart failure leading to enhanced vasoconstriction at rest and
decreased vasodilatation in response to exercise and ischemia, further contributing to heart failure (23).
Our findings of endothelial cell dysfunction in the lungs of our dogs
with chronic congestive heart failure concur with other reports in the
literature. Ontkeane et al. (23) reported decreased EDRF-mediated
relaxation to ACh in isolated PA rings taken from rats with congestive
heart failure. However, Mathew et al. (19) found no significant
difference in response to ACh and BK of canine pulmonary arteries
between pacing-induced congestive heart failure and control groups but
the vasodilatation to isoproterenol and prostacyclin was significantly
diminished. The differences between these findings and our study maybe
related to different neurohormonal activation of the heart failure
models. However, to our knowledge, this is the first report of complete
prevention or reversal of the pulmonary endothelial dysfunction with
treatment of an ACEI in MR dogs.
In summary, in dogs with chronic MR, pulmonary congestion results in a
significant decrease in the vasoconstrictor response to ANG II.
Furthermore, relaxation to BK in these pulmonary arteries is also
significantly decreased. These pulmonary vasomotion alterations are
normalized in dogs with MR treated with an ACEI. Dogs with MR
chronically treated with ramipril exhibit normal PA pressures in the
presence of normal ANG II sensitivity but increased peak ANG II
response. These in vitro and in vivo findings support the beneficial
use of ACEIs. Additionally, these results could suggest that BK-NO
signaling mechanisms may be important in pulmonary vasomotor tone in
heart failure and may supersede the vasoconstrictor effects of ANG II.
Whether these findings are applicable to the in vivo pulmonary
circulation requires further investigation.
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FOOTNOTES |
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: I. M. Straeter-Knowlen, Dept. of Medicine, Division of Cardiovascular
Disease, CNIR, 828 8th Court SO, Univ. of Alabama at Birmingham,
Birmingham, AL 35294-4470 (E-mail: ingridmari{at}aol.com).
Received 27 May 1998; accepted in final form 7 June 1999.
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