 -Adrenergic Stimulation Restores Rat Lung Ability to
Clear Edema in Ventilator-associated Lung Injury
Division of Pulmonary and Critical Care Medicine, Northwestern University Medical School, and Northeastern University, Chicago, Illinois; Departamento de Enfermedades Respiratorias, Pontificia Universidad Católica de Chile, Santiago, Chile
Mechanical ventilation with high tidal volume (HVT) causes
lung injury and decreases the lung's ability to clear edema in rats.
Pulmonary edema accumulates as the result of changes in hydrostatic or colloid-osmotic pressure gradients in the pulmonary circulation and/or increased permeability of the alveolocapillary barrier (1). Intermittent positive-pressure mechanical ventilation with high tidal volume (HVT) causes lung injury and pulmonary edema that mimics abnormalities observed in the acute respiratory distress syndrome (2). It has been reported that HVT ventilation increases microvascular filtration coefficient in isolated lungs (5) and produces a high permeability pulmonary edema in intact animals (6). It was also demonstrated that tidal volume excursion, and not peak airway pressure, is responsible for the pulmonary abnormalities associated with mechanical ventilation, which was accordingly named "volutrauma" rather than barotrauma (2, 7). Pulmonary edema formation in ventilator-associated lung injury (VALI) has been attributed to capillary stress failure, stretch pore phenomenon, depletion, and/or inactivation of surfactant constituents and release of proteolytic enzymes and proinflammatory mediators in the lung such as metalloproteinases and cytokines (8). Intermittent positive-pressure ventilation with high tidal volume and high inflation pressures (as much as 45 cm H2O) produces lung injury and pulmonary edema in rats (6, 7, 13). Recently, it has been reported that VALI decreases active Na+ transport, and lung edema clearance in association with downregulation of Na,K-ATPase activity in alveolar epithelial type II cells isolated from rats exposed to HVT ventilation for 40 min (14). It has been shown that This study was designed to determine whether
Pathogen-free, male, Sprague-Dawley rats weighing 280 to 320 g were
purchased from Harlan Sprague-Dawley, Inc. (Indianapolis, IN). A
total of 120 rat lungs were studied. All animals were provided food
and water ad libitum and maintained on a 12 h:12 h light-dark cycle.
Isoproterenol, terbutaline, amiloride, ouabain, choline chloride, colchicine, and Mechanical Ventilation Rats were anesthetized by intraperitoneal injection of 50 mg/kg body weight pentobarbital, tracheotomized, and mechanically ventilated in a rodent ventilator (Model 683; Harvard Apparatus, South Natick, MA). Adult rats were ventilated for 40 min with HVT of 40 ml/kg to peak airway pressures of 35 cm H2O and a respiratory rate of 40 breath/min and compared with control nonventilated rats. It has been previously reported that this experimental protocol causes lung injury and pulmonary edema and decreases active Na+ transport and lung edema clearance in rats (14). Specific Protocols Group A. Control group (n = 10 rats) instilled with 5 ml buffered salt albumin solution (BSA) into the air spaces. Group B. To examine Group C. Lung edema clearance in 10 rats exposed to HVT ventilation for 40 min. Group D. HVT ventilated rat lungs instilled with 10 Group E. To examine the alveolar epithelial Na+ transport pathway in rats exposed to HVT ventilation, we studied the effect of a Na+
channel blocker (amiloride 10 Group F. To determine whether there was significant edemagenises in HVT ventilated rat lungs as compared with control lungs, the lungs were instilled with a modified BSA solution. The BSA solution was modified by substituting sodium chloride with choline chloride (130.5 mM final concentration) (six in each group). Group G. We examined the contributory role of intracellular microtubular transport system on lung edema clearance modulation by
Isolated Lungs The isolated lung preparation was performed as previously described
(14, 18). Briefly, rats were anesthetized with 50 mg/kg body weight of
pentobarbital, tracheotomized, and mechanically ventilated with a
tidal volume of 2.5 ml, peak airway pressure of 8 to 10 cm H2O, and
100% oxygen for 5 min. The chest was opened via a median sternotomy, after which 400 U heparin sodium was injected into the right
ventricle. After exsanguination, the heart and lungs were removed en
bloc. The pulmonary artery and left atrium were catheterized, and the
pulmonary circulation was flushed of remaining blood by perfusing
with BSA solution containing in 135.5 mM Na+, 119.1 mM Cl Perfusion of the lungs was performed with 90 ml of the same BSA solution containing 0.16 mg/ml fluorescein-tagged albumin (FITC- albumin; Sigma). The perfusate was pumped from a lower reservoir to an upper reservoir by a peristaltic pump, and from there flowed through the pulmonary artery and exited via the left atrium. Pulmonary artery and left atria pressures were maintained at 12 and 0 cm H2O and recorded via a pressure transducer with a zero reference point at the level of the left atrium. Pulmonary artery and left atrium pressures were recorded continuously with a multichannel recorder (Gould 3000 Oscillograph Recorder; Gould Inc., Cleveland, OH). Pulmonary circulation pressures and flow rates were measured periodically during the experiments. Samples were drawn from the three reservoirs: air-space instillate, "pleural bath," and perfusate at 10 and 70 min after starting the experimental protocol. To ensure homogeneous sampling from the air spaces, 2 ml of instillate were aspirated and reintroduced into the air spaces three times before removing each sample. This has been shown to provide a reproducibly mixed sample in our laboratory and in previous work (14, 18). All samples were centrifuged at 1,000 × g for 15 min. Colorimetric analysis of the supernatant for EBD (absorbance at 620 nm) was performed in a Hitachi Model U2000 Spectrophotometer (Hitachi Inst., San Jose, CA). Analysis of FITC-albumin (excitation 487 nm and emmission 520 nm) was performed in a Perkin-Elmer fluorescence spectrometer (Model LS-3B; Perkin-Elmer, Oakbrook, IL). 22Na+ and 3H-mannitol were measured in a betacounter (Packard Tricarb; Packard Instrument Co., Downers Grove, IL). Calculations The alveolar lining fluid volume (VELF) was calculated by instilling 3 ml of fluid (V0) containing a known concentration of albumin (EBD)0, tagged by Evans blue dye into the air space. After brief mixing, a sample was removed and the Evans blue dye concentration at time t (EBD)t was estimated. The amount of Evans blue dye is the same in the instillate [V0(EBD)0] and in the lung after initial mixing [(V0 + VELF)(EBD)t]. Equating the two yields:
Similarly, the alveolar fluid volume at time t is estimated by:
The movement of sodium for the alveolar space during a defined
period of time is assumed to be accompanied by isotonic water flux and
is given by: JNa,net = JNa,out
As described by Rutschman and colleagues (25), the passive movement of 22Na+, JNa,in, is given by :
where C(x) is the 22Na+ concentration at time x and [Na+] is the constant Na+ concentration in the BSA solution. Similarly, the volume flux of mannitol (typically expressed as PA, permeability-surface area product) is given by:
where M(x) is the [3H]mannitol mass at time x. Albumin flux from the pulmonary circulation into the alveolar space was determined from the fraction of FITC-albumin that appears in the alveolar space during the experimental protocol. These calculations were carried out for each sampling period. ATII Cell Isolation, Total RNA Isolation, and RT-PCR Analysis ATII cells were isolated from adult rat lungs as previously described (14, 18). Briefly, the lungs were perfused via the pulmonary artery, lavaged, and digested with elastase 30 U/ml (Worthington Biochemical Corp., Freehold, NJ) for 20 min at 37° C. the tissue was minced and filtered through sterile gauze and 70-µm nylon mesh. The crude cell suspension was purified by differential adherence to immunoglobulin G-pretreated dishes, and cell viability was assessed by trypan blue exclusion (> 95%). Total cellular RNA was extracted from ATII cells isolated from
control rats and rats exposed to HVT for 40 min that were incubated with 1 µM ISO for 60 min, using RNeasy total RNA kit (Qiagen Inc., Santa Clarita, CA), as described by the manufacturer, based on the
method described by Chomczynski and Sacchi (26). RNA was quantified by measurement of absorbance at 260 nm. The reverse transcriptase (RT) reaction was performed using the Superscript Preamplification System (GIBCO-BRL, Gaithersburg, MD) following the
manufacturer's instructions. Briefly, 1 µg of total RNA was converted
into cDNA, after denaturing at 70° C for 15 min, by incubation with a
buffer containing oligo-dT primers, the reverse transcriptase (RT) enzyme, and dNTPs mix for 50 min at 42° C. The RT enzyme was then
inactivated by incubation at 70° C for 15 min and the RNA removed
by incubation with RNAse H for 20 min at 37° C. The resultant cDNAs
were amplified by PCR using a Perkin Elmer 4800 Thermal Cycler
(Perkin Elmer-Cetus, Norwalk, CT). Specific primers for the Na,K-ATPase
Data Analysis Data are presented as mean values ± SEM. When comparisons were made between two experimental groups Student's unpaired t test was used. When multiple comparisons were made a one-way analysis of variance was used, followed by a multiple comparison test (Tukey) when the F statistic indicated significance. Results were considered significant at p < 0.05.
Epithelial Permeability The epithelial lining fluid (ELF) volume, estimated by the dilution of EBD in the first BAL, did not change significantly in rats ventilated with HVT for 40 min (Table 2). However, alveolar epithelial permeability to small solutes (22Na+ and 3H-mannitol) increased in rats ventilated with HVT for 40 min as compared with control nonventilated rats. As shown in Table 2, and as previously reported, isoproterenol and terbutaline mildly increased the passive flux of small solutes in control nonventilated rats (16, 18).
The movement of albumin across the alveolar epithelial
barrier was small, similar to the previously reported rates in
normal rat lungs (14, 16, 18, 22, 25). Evans Blue dye-bound albumin instilled in the air space was not detected in the perfusate or bath compartments in any of the experimental groups.
The movement of FITC-albumin from the pulmonary circulation into air space was minimal and not affected by HVT ventilation or Lung Edema Clearance Terbutaline instilled into the air spaces and isoproterenol perfused through the pulmonary circulation increased lung edema clearance ~ 60 to 100% over basal levels in control nonventilated rats (from 0.50 ± 0.02 ml/h to 0.81 ± 0.04 ml/h and 0.99 ± 0.05 ml/h, respectively) (Figure 1). In ventilator- associated lung injury, active Na+ transport and lung edema clearance decreased by ~ 50% when compared with control rats (p < 0.001). TERB and ISO restored the lung's ability to clear edema in rats exposed to HVT ventilation for 40 min (from 0.25 ± 0.03 ml/h to 0.64 ± 0.02 ml/h and 0.88 ± 0.09 ml/h, respectively) (Figure 1). To determine that the decrease in lung edema clearance was due to changes in the active Na+ transport and not to edema accumulation, choline chloride was iso-osmotically substituted for sodium chloride in the BSA. As shown in Figure 2, in the lungs ventilated with HVT and instilled with choline chloride, there was no fluid reabsorption, as Na+ is needed to drive active Na+ transport and clearance. Additionally, there was no fluid accumulation, confirming that at the low hydrostatic pressures across the pulmonary circulation utilized in our model there was no edema formation.
The Na+ channel blocker amiloride and the Na,K-ATPase
antagonist ouabain inhibited the stimulatory effect of ISO in
HVT ventilated rats (Figure 3). Pulmonary circulation flow
rates were not affected by
We examined the contributory role of the cellular microtubular transport system on
We also studied whether the Na,K-ATPase
Mechanical ventilation is frequently used to support the ventilatory function of patients with acute hypoxemic respiratory failure and pulmonary edema. However, it has been reported that mechanical ventilation with high inflation pressures and high tidal volumes can cause capillary stress fracture of the alveolocapillary barrier, depletion or inactivation of surfactant components, and release of proinflammatory mediators, which causes leakage of fluid, protein, and blood constituents into the lung interstitium and alveolar spaces (2, 8). Therefore, artificial ventilatory support may potentially worsen the pulmonary function by causing alveolar overdistension, especially in patients with acute respiratory distress syndrome and preexisting injured lungs (2). Positive-pressure ventilation of rats with high tidal volumes
for short periods of time produces lung injury and high permeability pulmonary edema (6, 7, 13). In this model, the increased tidal volume excursions, and not peak airway pressures, increase pulmonary microvascular filtration and extravascular
lung water (7). It has been reported that adult rats ventilated
with high tidal volume (40 ml/kg and to peak airway pressures
of 35 cm H2O) for 40 min causes lung injury and decreases alveolar fluid reabsorption, in association with downregulation
of alveolar epithelial Na,K-ATPase function (14). In the present study, we examined whether the It has also been suggested that isoproterenol could attenuate high permeability pulmonary edema and reduce pulmonary vascular permeability by stabilization of the endothelial
cell cytoskeleton (29, 30). Parker and Ivey (29) have reported
that isoproterenol significantly attenuates increases in high
vascular pressure-induced capillary filtration coefficient (Kfc).
These effects are probably mediated by higher intracellular
cAMP levels and by inhibiting the active ATP and Ca+2-
dependent contraction of cytoskeleton myofibrils in endothelial and epithelial cells (29). However, ISO and TERB did not
significantly affect alveolocapillary barrier permeability in
VALI-exposed rats (see Table 1). Therefore, To examine the active Na+ transport pathway in rat alveolar epithelium, we studied the effects of the Na+ channel
blocker amiloride and the Na,K-ATPase antagonist ouabain in rats exposed to VALI. Both amiloride and ouabain inhibited the stimulatory effects of ISO on lung edema clearance in
rats ventilated with HVT, suggesting that The sodium pump plays a critical role translocating sodium
molecules against an electrochemical gradient in the alveolar
epithelium (14, 18, 20, 27). The Na,K-ATPase may be regulated at different levels, including transcription, translation,
protein degradation rate, recruitment from intracellular pools
to the plasma membrane, recycling from the plasma membrane, and structural changes of Na+ pumps in the plasma
membrane (32, 33). It has been shown that Finally, alveolar epithelial Na,K-ATPase In conclusion, we have shown that
Correspondence and requests for reprints should be addressed to J. I. Sznajder, M.D., Department of Medicine, Northwestern University, 300 East Superior, Tarry 14-707, Chicago, IL 60611. (Received in original form September 14, 1998 and in revised form December 17, 1999). Acknowledgments: Supported in part by Grant HL-48129 from the National Institutes of Health, Grant 96012890 from the American Heart Association, FONDECYT 1990515, and Universidad Católica de Chile.
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ABSTRACT
INTRODUCTION
-adrenergic agonists increase active Na+ transport and lung
edema clearance in normal rat lungs by stimulating apical Na+
channels and basolateral Na,K-ATPase in alveolar epithelial cells. We studied whether 
1- and 
5 M TERB was instilled into the air spaces
or 10
JNa,in, where JNa,net is the net or active Na+
transport, JNa,out is the total or unidirectional Na+ out flux from the rat
air spaces, and JNa,in is the passive bidirectional flux of Na+ between the
air space and the other compartments. The volume flux J = JNa,net/
[Na+] is the average rate of change in the volume and is given by:
![J<SUB>Na,in</SUB>=[Na<SUP>+</SUP>] J (ln C<SUB>(t)</SUB>−ln C<SUB>(0)</SUB>)/(ln V<SUB>t</SUB>−ln V<SUB>0</SUB>)](/content/vol162/issue1/fulltext/282/img005.gif)
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  G. M. Mutlu and P. Factor Alveolar Epithelial 2-Adrenergic Receptors Am. J. Respir. Cell Mol. Biol., February 1, 2008; 38(2): 127 - 134. [Abstract] [Full Text] [PDF]
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 J. A. Frank, R. Briot, J. W. Lee, A. Ishizaka, T. Uchida, and M. A. Matthay Physiological and biochemical markers of alveolar epithelial barrier dysfunction in perfused human lungs Am J Physiol Lung Cell Mol Physiol, July 1, 2007; 293(1): L52 - L59. [Abstract] [Full Text] [PDF]
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 J. Litvan, A. Briva, M. S. Wilson, G. R. S. Budinger, J. I. Sznajder, and K. M. Ridge beta-Adrenergic Receptor Stimulation and Adenoviral Overexpression of Superoxide Dismutase Prevent the Hypoxia-mediated Decrease in Na,K-ATPase and Alveolar Fluid Reabsorption J. Biol. Chem., July 21, 2006; 281(29): 19892 - 19898. [Abstract] [Full Text] [PDF]
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 M. Cepkova and M. A. Matthay Pharmacotherapy of Acute Lung Injury and the Acute Respiratory Distress Syndrome J Intensive Care Med, May 1, 2006; 21(3): 119 - 143. [Abstract] [PDF]
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J. S. Steingrub Adding Up the Zeros J Intensive Care Med, May 1, 2006; 21(3): 188 - 190. [PDF]
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G. M. Mutlu and J. I. Sznajder Mechanisms of pulmonary edema clearance Am J Physiol Lung Cell Mol Physiol, November 1, 2005; 289(5): L685 - L695. [Abstract] [Full Text] [PDF]
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 G. M. Mutlu, W. J. Koch, and P. Factor Alveolar Epithelial {beta}2-Adrenergic Receptors: Their Role in Regulation of Alveolar Active Sodium Transport Am. J. Respir. Crit. Care Med., December 15, 2004; 170(12): 1270 - 1275. [Full Text] [PDF]
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C. P. Thomas, J. R. Campbell, P. J. Wright, and R. F. Husted cAMP-stimulated Na+ transport in H441 distal lung epithelial cells: role of PKA, phosphatidylinositol 3-kinase, and sgk1 Am J Physiol Lung Cell Mol Physiol, October 1, 2004; 287(4): L843 - L851. [Abstract] [Full Text] [PDF]
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 J. M. Liebler, Z. Borok, X. Li, B. Zhou, A. J. Sandoval, K.-J. Kim, and E. D. Crandall Alveolar Epithelial Type I Cells Express {beta}2-Adrenergic Receptors and G-protein Receptor Kinase 2 J. Histochem. Cytochem., June 1, 2004; 52(6): 759 - 767. [Abstract] [Full Text] [PDF]
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G. Saumon Pump and Circumstances Am. J. Respir. Crit. Care Med., December 15, 2003; 168(12): 1408 - 1409. [Full Text] [PDF]
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Y. Adir, P. Factor, V. Dumasius, K. M. Ridge, and J. I. Sznajder Na,K-ATPase Gene Transfer Increases Liquid Clearance during Ventilation-induced Lung Injury Am. J. Respir. Crit. Care Med., December 15, 2003; 168(12): 1445 - 1448. [Abstract] [Full Text] [PDF]
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 E. Lecuona, K. Ridge, L. Pesce, D. Batlle, and J. I. Sznajder The GTP-binding Protein RhoA Mediates Na,K-ATPase Exocytosis in Alveolar Epithelial Cells Mol. Biol. Cell, September 1, 2003; 14(9): 3888 - 3897. [Abstract] [Full Text] [PDF]
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M. Sugita, P. Ferraro, A. Dagenais, M.-E. Clermont, P. Barbry, R. P. Michel, and Y. Berthiaume Alveolar Liquid Clearance and Sodium Channel Expression Are Decreased in Transplanted Canine Lungs Am. J. Respir. Crit. Care Med., May 15, 2003; 167(10): 1440 - 1450. [Abstract] [Full Text] [PDF]
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J. A. Frank, J.-F. Pittet, H. Lee, M. Godzich, and M. A. Matthay High tidal volume ventilation induces NOS2 and impairs cAMP- dependent air space fluid clearance Am J Physiol Lung Cell Mol Physiol, May 1, 2003; 284(5): L791 - L798. [Abstract] [Full Text] [PDF]
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D. E. Schraufnagel, N. P. Agaram, A. Faruqui, S. Jain, L. Jain, K. M. Ridge, and J. I. Sznajder Pulmonary lymphatics and edema accumulation after brief lung injury Am J Physiol Lung Cell Mol Physiol, May 1, 2003; 284(5): L891 - L897. [Abstract] [Full Text] [PDF]
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 K.M. Ridge, W.G. Olivera, F. Saldias, Z. Azzam, S. Horowitz, D.H. Rutschman, V. Dumasius, P. Factor, and J.I. Sznajder Alveolar Type 1 Cells Express the {alpha}2 Na,K-ATPase, Which Contributes to Lung Liquid Clearance Circ. Res., March 7, 2003; 92(4): 453 - 460. [Abstract] [Full Text] [PDF]
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 Y. Berthiaume, H. G. Folkesson, and M. A. Matthay Lung Edema Clearance: 20 Years of Progress: Invited Review: Alveolar edema fluid clearance in the injured lung J Appl Physiol, December 1, 2002; 93(6): 2207 - 2213. [Abstract] [Full Text] [PDF]
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 M. A. Matthay Alveolar Fluid Clearance in Patients With ARDS: Does It Make a Difference? Chest, December 1, 2002; 122(6_suppl): 340S - 343S. [Abstract] [Full Text] [PDF]
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 C. Sartori and M.A. Matthay Alveolar epithelial fluid transport in acute lung injury: new insights Eur. Respir. J., November 1, 2002; 20(5): 1299 - 1313. [Abstract] [Full Text] [PDF]
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J. I. Sznajder, P. Factor, and D. H. Ingbar Lung Edema Clearance: 20 Years of Progress: Invited Review: Lung edema clearance: role of Na+-K+-ATPase J Appl Physiol, November 1, 2002; 93(5): 1860 - 1866. [Abstract] [Full Text] [PDF]
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M. A. Matthay, C. Clerici, and G. Saumon Lung Edema Clearance: 20 Years of Progress: Invited Review: Active fluid clearance from the distal air spaces of the lung J Appl Physiol, October 1, 2002; 93(4): 1533 - 1541. [Abstract] [Full Text] [PDF]
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J. L. Fisher and S. S. Margulies Na+-K+-ATPase activity in alveolar epithelial cells increases with cyclic stretch Am J Physiol Lung Cell Mol Physiol, October 1, 2002; 283(4): L737 - L746. [Abstract] [Full Text] [PDF]
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F. J. Saldias, A. P. Comellas, L. Pesce, E. Lecuona, and J. I. Sznajder Dopamine increases lung liquid clearance during mechanical ventilation Am J Physiol Lung Cell Mol Physiol, July 1, 2002; 283(1): L136 - L143. [Abstract] [Full Text] [PDF]
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 C. Sartori, Y. Allemann, H. Duplain, M. Lepori, M. Egli, E. Lipp, D. Hutter, P. Turini, O. Hugli, S. Cook, et al. Salmeterol for the Prevention of High-Altitude Pulmonary Edema N. Engl. J. Med., May 23, 2002; 346(21): 1631 - 1636. [Abstract] [Full Text] [PDF]
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K. M. Hardiman and S. Matalon Modification of Sodium Transport and Alveolar Fluid Clearance by Hypoxia . Mechanisms and Physiological Implications Am. J. Respir. Cell Mol. Biol., November 1, 2001; 25(5): 538 - 541. [Full Text] [PDF]
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M. J. TOBIN Critical Care Medicine in AJRCCM 2000 Am. J. Respir. Crit. Care Med., October 15, 2001; 164(8): 1347 - 1361. [Full Text] [PDF]
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H. E. Dincer, N. Gangopadhyay, R. Wang, and B. D. Uhal Norepinephrine induces alveolar epithelial apoptosis mediated by {alpha}-, {beta}-, and angiotensin receptor activation Am J Physiol Lung Cell Mol Physiol, September 1, 2001; 281(3): L624 - L630. [Abstract] [Full Text] [PDF]
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J. I. Sznajder Alveolar Edema Must Be Cleared for the Acute Respiratory Distress Syndrome Patient to Survive Am. J. Respir. Crit. Care Med., May 1, 2001; 163(6): 1293 - 1294. [Full Text]
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