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ABSTRACT |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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Red blood cell (RBC) transfusion is usually administered to improve oxygen delivery (DO2) in order to sustain tissue oxygen demand. However, this practice is not supported by firm clinical or
experimental data. Using a randomized two-period crossover design, this study compared the efficacy of "fresh" RBC transfusion and increased blood flow to restore tissue oxygenation in oxygen supply-dependent conditions. In 12 ketamine-anesthetized mongrel dogs submitted to nonpulsatile normothermic cardiopulmonary bypass, DO2 was reduced by a progressive decrease in pump
flow. DO2 dependency was defined as an O2 uptake (
O2) decrease
by more than 15% from baseline value. Then, intervention consisted of a 40% increase in DO2 obtained either by transfusion of
"fresh" dog's RBC (stored < 3 d) or by increase in pump flow. Animals received both interventions sequentially in a random order,
while O2 saturation was maintained constant. In O2 supply-dependent conditions, rising pump flow from 1.6 ± 0.4 to 2.7 ± 0.7 L/
min increased DO2 from 5.4 ± 1.1 to 9.0 ± 1.3 ml/kg/min (p < 0.01) and O2 from 3.5 ± 0.4 to 4.1 ± 0.5 ml/kg/min (p = 0.02).
"Fresh" RBC transfusion, which increased the hemoglobin concentration from 6.4 ± 0.9 to 11.1 ± 1.3 g/dl, increased DO2 from 5.4 ± 1.2 to 9.0 ± 1.4 ml/kg/min (p < 0.01) and O2 from 3.6 ± 0.4 to
4.1 ± 0.5 ml/kg/min (p = 0.02). There was no difference in O2 resulting from both interventions. In oxygen supply-dependent conditions, "fresh" RBC transfusion and increased blood flow are
equally effective in restoring tissue oxygenation.
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INTRODUCTION |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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In critically ill patients, the major indication for red blood cell (RBC) transfusion is the correction or the improvement of oxygen delivery to sustain tissue oxygen demand (1). However, this practice is not supported by firm clinical or experimental data. On the contrary, blood transfusion may affect the different determinants of the oxygen delivery-oxygen uptake relationship. First, blood transfusion is not always associated with an increase in oxygen delivery (2). The rise in oxygen-carrying capacity may indeed be counterbalanced by a decrease in blood flow, secondary to a higher blood viscosity. Second, even in the presence of an increased oxygen delivery, blood transfusion is not always associated with an increased oxygen uptake. This has been attributed to either the absence of oxygen deficit or to the inability of blood transfusion to correct a debt in tissue oxygenation (3). Evaluation of blood transfusion effects on oxygen uptake therefore requires situations in which oxygen uptake-oxygen delivery dependency can be identified. Even if blood transfusion would prove to be effective in restoring oxygen uptake in these conditions, its relative efficacy has to be compared with other standard forms of treatment such as increasing blood flow. Indeed, from a physiological point of view, increases in blood flow could theoretically augment the perfused capillary area by increases in filling pressures or microvascular vasodilation, resulting in increased oxygen uptake. The effects of blood transfusion on oxygen uptake may be less predictable than the effect of blood flow as the rise in hematocrit will increase blood viscosity, which may alter regional microvascular blood flow (4).
The present study addressed this issue in a model of oxygen uptake-oxygen supply dependency during cardiopulmonary bypass in anesthetized dogs. Providing a similar increase in oxygen delivery, the effects of "fresh" red blood cell transfusion on oxygen uptake were compared with those of an increase in blood flow.
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METHODS |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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Anesthesia and Surgical Preparation
All experimental procedures used in this investigation were performed according to the NIH guidelines and were approved by the Erasme Institutional Animal Investigation Committee. The study included 12 mongrel dogs (27.6 ± 3.7 kg). After 12 h of fasting, animals were anesthetized with an intravenous administration of 5 mg/kg of ketamine. Endotracheal intubation was performed, and mechanical ventilation was started (Elema 900 B; Siemens, Solna, Sweden) with air (fraction of inspired oxygen [FIO2] = 0.21). The respiratory rate was set at 12/min and the tidal volume was adapted to obtain a PaCO2 between 35 and 40 mm Hg. Anesthesia was maintained with a continuous infusion of ketamine at 0.2 mg/kg/min and pancuronium bromide at 0.1 mg/kg followed by repeated boluses of 1 to 2 mg/h. A femoral artery catheter was advanced into the abdominal aorta through the right femoral artery for arterial pressure monitoring and blood gas analysis. In each animal, hemoglobin concentration was lowered to 10 g/dl by normovolemic hemodilution. The blood withdrawn was replaced by the same volume of 4% modified fluid gelatin (Gelofusin; Braun, Melsungen, Germany). In these acute conditions, modified fluid gelatin has been found as efficient as low molecular starch in maintaining intravascular volume (5).
A median sternotomy was performed. After administration of 5 mg/ kg of heparin, cannulas were inserted in the aortic root and the right atrial appendage. The blood circulation was maintained by a roller pump (Stöckert Instrumente GmbH, München, Germany) through a combined pediatric heat-exchanger-oxygenator (Midiflo D705; Sorin Dideco, Mirandola, Italy). The CPB circuit was primed with 4% modified fluid gelatin (Gelofusin; Braun). The prime volume was adjusted to obtain a hemoglobin concentration of 6 g/dl on cardiopumonary bypass. Sodium bicarbonate was added to obtain a pH about 7.35. After controlling the anticoagulation (activated coagulation time [ACT] greater than 450 s), the bypass was started at a flow of 120 ml/kg/min. The aorta was then clamped and the heart stopped using 200 ml of cardioplegic solution (Ringer lactate with 30 mEq/L potassium chloride). A left ventricular venting sump was then inserted. Cardiopulmonary bypass was performed at 38° C. Gas flow and FIO2 were adapted throughout the experiment to maintain a PaCO2 between 30 and 35 mm Hg and a PaO2 above 100 mm Hg. Mixed venous O2 saturation (SvO2) was continuously monitored (Oxystat SW0200 monitor; Baxter-Bentley, Irvine, CA). To compensate for insensible water losses during the experimental procedure, each dog received a saline infusion given at a rate of 10 ml/kg during the first hour and 1 ml/kg/h thereafter. Throughout the experimental procedure, additional volumes of gelatin were administered into the venous reservoir to maintain the hemoglobin level of 6 g/dl. ACT was maintained above 450 s throughout the entire procedure by additional doses of heparin (1-2 mg/kg).
After aortic cross-clamping, a period of 15 min was allowed to achieve steady state, defined by a stable mean arterial pressure and SvO2. Baseline measurements of arterial pressure and pump flow were then recorded. Immediately thereafter, arterial and venous blood samples were drawn from the arterial and venous lines for the measurement of blood gas tensions (ABL 2; Radiometer, Copenhagen, Denmark). Hemoglobin concentration and oxygen saturation were measured by cooximetry, with the instrument calibrated for canine blood (OSM3; Radiometer). Each sample was analyzed at least twice, with a variability between measurements less than 5%. Serum lactate concentration was assessed enzymatically by an automated analyzer (Kontron, Basel, Switzerland).
Total vascular resistance (TVR), arterial oxygen content (CaO2),
mixed venous oxygen content (CvO2), DOO2, O2, oxygen extraction ratio (O2ER), and venoarterial gradient for PCO2 (VAPCO2) were calculated using the following formulas:
TVR (d/s/cm5) = (mean arterial pressure [MAP]/pump flow) × 79.9
CaO2 (m/dl) = (Hb × 1.39 × SaO2) + (0.0031 × PaO2)
CvO2 (m/dl) = (Hb × 1.39 × SvO2) + (0.0031 × PvO2)
DO2 (ml/kg/min) = (pump flow × CaO2 × 10) /weight
O2(ml/kg.min) = (pump flow × [CaO2 
CvO2] × 10)/weight
O2ER (%) = (CaO2 CvO2)/CaO2
VAPCO2 (mm Hg) = PvCO2 PaCO2
Experimental Protocol
After baseline measurements, oxygen delivery was reduced by a progressive decrease in pump flow by steps of 10 ml/kg/min. At each step,
a 10-min period was allowed to achieve a new steady state before another set of measurements was performed. At the same time, O2 and
DO2 were calculated. Oxygen supply dependency was considered to
be present when two successive experimental steps showed a decrease
in calculated O2 value. This particular point, corresponding to a O2
value of 15-20% below baseline, was defined as control 1.
The experimental protocol is illustrated in Figure 1. A randomized
two-period crossover design with baseline measurements was used in
this study. All animals were subjected to two consecutive different interventions, to obtain an increase in systemic oxygen supply of at least
40%. These interventions consisted of either an augmentation in
pump flow or an increase in hemoglobin concentration obtained by
the transfusion of "fresh" dog red blood cells (stored in citrate phosphate adenine for less than 3 d). Dogs were randomized according to
the order of administration of the two consecutive interventions. After the first intervention, either pump flow or hemoglobin level was
returned to the values obtained in the control 1 conditions (control 2)
before the second was administered. After the second intervention,
pump flow or the hemoglobin level was again returned to the control
1 condition values (control 3). Hemoglobin level was decreased by
normovolemic hemodilution using dog's plasma and 4% modified
fluid gelatin. At this point, oxygen delivery was further decreased by a
progressive reduction in pump flow to approximately 20 ml/kg/min to
define the complete O2-DO2 relationship. Serum lactate was measured at each time point, except during the two intervention periods.
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In each animal, the O2-DO2 relationship was analyzed from all experimental points. Critical DO2, defined as the DO2 value below which
O2 becomes DO2 dependent, was determined using the mathematical
analysis developed by Samsel and Schumacker (6). Briefly, paired sets
of linear regressions were calculated, after sorting the DO2 and O2
paired values with increasing DO2 for all possible combinations of
points separated into low (supply-dependent) and high (supply-independent) DO2 groups. Points were constrained to fall on either regression line, but never on both. The pair of regressions with the lowest sum
of the standard errors of estimate was taken as the set that best fit the
data. The values of DO2 and O2 at the intersection point were than calculated using the two regression equations. The extraction ratio at the
critical point was calculated by dividing O2crit by DO2crit. The critical value of DO2 was also determined in each animal from a plot of serum
lactate versus DO2 using the same computing method described above.
Statistical Analysis
The statistical analysis of the effects of the two interventions consisted in an analysis of variance for a 2 × 2 crossover design with baseline measurements (7). First, carryover effects (first order and second order) were tested. As carryover effects were not significant, data after treatment from both periods were combined and compared using an analysis of variance for repeated measures. If the F value reached the level of significance, pairwise comparisons were made, using a Tukey's Honestly Significant Difference test. For all tests, a p value < 0.05 was considered significant. All values are expressed as mean ± SD.
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RESULTS |
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ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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Table 1 shows data obtained at the beginning (baseline) at the
critical point and at the end of the experiments and data at the
critical point. In our study conditions, critical DO2 was 6.6 ± 1.8 ml/kg/min. Critical DO2 obtained from lactate concentrations was similar to the one identified from O2 measurements
(6.4 ± 2.0 ml/kg/min).
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Data obtained before and after each intervention are presented in Table 2. Two different interventions were applied to
animals in oxygen supply-dependent conditions to obtain an
increase in DO2 of at least 40%. The first intervention consisted of an increase in pump flow from 1.64 ± 0.44 to 2.73 ± 0.67 L/min (p < 0.001), while arterial oxygen content was
maintained constant (Table 2, column T2). This intervention
resulted in a significant increase in MAP, while TVR did not
change. The second intervention consisted of an increase in
hemoglobin concentration from 6.4 ± 0.9 to 11.1 ± 1.3 g/dl (p < 0.001), while pump flow and arterial oxygen saturation were
maintained constant (Table 2, column T4). This intervention resulted in a significant increase in MAP and in TVR. TVR was also significantly higher after the hemoglobin increase than after the pump flow increase. Both interventions were associated
with a similar increase in DO2 resulting in a similar increase in
O2, back to the supply-independent part of the O2-DO2 relationship (Table 2 and Figure 2). The venoarterial gradient for
PCO2 decreased in a similar manner with the two interventions.
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DISCUSSION |
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TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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In conditions of oxygen supply dependency, a similar increase in oxygen delivery, either by transfusion of "fresh" red blood cells or increment in pump flow, resulted in a similar increase in oxygen uptake.
Numerous studies have addressed the effects of red blood
cell transfusion on tissue oxygenation in critically ill patients, with conflicting results (3, 8). Differences in experimental design were obviously confounding factors. However, the absence of a clear demonstration of a O2-DO2-dependent status
was a major weakness in these studies. Only when transfusion
is carried out in this condition is red blood cell administration
expected to increase tissue oxygenation.
Two recent experimental studies specifically address this issue. In rats placed into supply dependency conditions by hemodilution, Fitzgerald and coworkers (12) and Sielenkämper and coworkers (13) demonstrated that "fresh" (stored for less than 6 d) red blood cell transfusion improved tissue oxygenation. The present study shows similar results in dogs placed into supply-dependency conditions during cardiopulmonary bypass. Moreover, our data demonstrate that "fresh" red blood cell transfusion was as efficacious as an increase in blood flow not only to improve oxygen delivery, but also to restore oxygen uptake. The effects of hematocrit on oxygen uptake may be less predictable than the effect of blood flow. Indeed, the rise in hematocrit will be associated with an increase in blood viscosity, which in turn may alter blood flow distribution at the capillary level. Using intravital microscopy, Vicaut and coworkers (14) showed that hemoconcentration to a hematocrit of 55% did not modify capillary density but was associated with an increase in the number of capillaries containing stationary red blood cells. These results illustrate that acute hemoconcentration increases the heterogeneity of capillary perfusion by excluding capillaries with high hematocrit from perfusion (4). However, at all shear rates, the relationship between hematocrit and whole blood viscosity is exponential. This might explain why increasing the hemoglobin level within the normal physiological range to improve oxygen delivery resulted in a similar increase in oxygen uptake than an increase in blood flow.
Our results are in contrast to those reported by Lorente and coworkers (15). In patients presenting a supply-dependent oxygen uptake, only increase in blood flow by dobutamine was able to improve tissue oxygenation, in opposition to transfusion of allogeneic units of red blood cells. However, improvement in oxygen delivery resulting from these two treatments was not equivalent. Furthermore, by its direct calorigenic effects, dobutamine could also increase oxygen uptake (16). Finally, the authors did not specify the age of the red blood cells they used to increase oxygen supply. Importantly, it has been shown that only "fresh" red blood cell transfusion and not old (> 28 d storage) improved tissue oxygenation in oxygen supply-dependent conditions (12, 13). The apparent inefficacy of old red blood cell transfusion to increase oxygen uptake has been attributed to a 2-3 diphosphoglycerate depletion and to the decreased deformability of the red blood cells (17- 19). These two "storage" effects would result in a relative inability of old red blood cells to increase oxygen delivery at the cellular level. Our results may have clinical implications regarding the therapeutic approach when acute improvements in tissue oxygenation are required. Future studies have to determine whether it is preferable to use fresh red blood cells in this setting and to evaluate treatments that either protect or restore red blood cell properties before transfusion.
To evaluate the effects of "fresh" red blood cell transfusion on oxygen uptake, we need an experimental model in which the different determinants of oxygen delivery could be accurately controlled. We therefore used a cardiopulmonary bypass model. Critical oxygen delivery observed in this model is somewhat lower than that obtained with other models, such as hemorrhagic shock, anemia, or cardiac tamponade (5, 20). Our model is distinguished from these because it excludes the heart and lungs from the systemic circulation and because it uses nonpulsatile blood flow. As for other models, critical oxygen delivery obtained from lactate measurements was comparable to the one estimated from oxygen uptake measurements (5, 23, 26, 27).
Several points deserve discussion. Anesthesia was maintained with ketamine. Anesthetic agents have been shown to
alter the O2-DO2 relationship in a dose-dependent manner
(23). Among these agents, ketamine appeared to have the
least effects on this relationship. This is probably because of
its stimulant properties on the central nervous system (28).
Oxygen supply dependency was defined when two successive experimental points showed a decrease in calculated oxygen uptake. Oxygen delivery and oxygen uptake at the different control points (Table 2) were consistently 15-20% below critical values (Table 1). This indicated that interventions were administered when animals were in supply-dependent conditions.
Interventions aimed at an increase in systemic oxygen delivery by at least 40%. This end point was chosen to ensure improvement in oxygen delivery far above the calculated critical point. With such an increase, possible confounding factors related to a mathematical coupling between oxygen delivery and oxygen uptake determination were minimized. Moreover, to reduce possible errors as a consequence of mathematical coupling, we used the same model of tubing in the pump circuit for all experiments. Pump flow was measured electronically and was validated by a stroboscopic device. Direct measurement of oxygen consumption using a metabolic cart would have been a means of confirming the effects of DO2 changes in oxygen uptake. However, membrane oxygenators presented a significant air leak that precluded any reliable measurement of oxygen consumption.
In conclusion, in oxygen supply-dependent conditions, "fresh" RBC transfusion and increased blood flow are equally effective in restoring tissue oxygenation.
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Footnotes |
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Correspondence and requests for reprints should be addressed to Philippe Van der Linden, M.D., Ph.D., Department of Cardiac Anesthesia, CHU Charleroi, 73 route de Gosselies, B-6040 Jumet, Belgium. E-mail: pvanderlinden{at}skynet.be
(Received in original form January 3, 2000 and in revised form February 26, 2001).
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References |
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ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES
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1.
Hébert CA,
Wells GA,
Blajchman MA,
Marshall J,
Martin C,
Pagliarello G,
Tweedale M,
Schweitzer I,
Yetisir E.
A multicenter randomized controlled clinical trial of transfusion requirements in critical
care.
N Engl J Med
1999;
340:
409-417
2. Heyland DK, Cook DJ, King D, Kenerman P, Brun Buisson C. Maximizing oxygen delivery in critically ill patients: a methodologic appraisal of the evidence. Crit Care Med 1996;24:517-524.
3.
Marik PE,
Sibbald WJ.
Effects of stored blood transfusion on oxygen delivery in patients with sepsis.
JAMA
1993;
269:
3024-3029
4. Messmer K. Blood rheology factors and capillary blood flow. In: Guttierrez G, Vincent JL, editors. Tissue oxygen utilization. Berlin, Heidelberg: Springer-Verlag; 1991. p. 103-113.
5.
Van der Linden P,
Schmartz D,
De Groote F,
Mathieu N,
Willaert P,
Rausin I,
Vincent JL.
Critical haemoglobin concentration in anaesthetized dogs: comparison of two plasma substitutes.
Br J Anaesth
1998;
81:
556-562
6.
Samsel RW,
Schumacker PT.
Determination of the critical O2 delivery
from experimental data: sensitivity to error.
J Appl Physiol
1988;
64:
2074-2082
7. Jones B, Kenward MG. Design and analysis of cross-over trials. London, UK: Chapman and Hall; 1989. p. 60-67.
8. Lucking SE, Williams TM, Chaten FC, Metz RI, Mickell JJ. Dependence of oxygen consumption on oxygen delivery in children with hyperdynamic septic shock and low oxygen extraction. Crit Care Med 1990; 18: 1316-1319 [Medline].
9. Mink RB, Pollack MM. Effect of blood transfusion on oxygen consumption in pediatric septic shock. Crit Care Med 1999; 18: 1087-1091 .
10. Dietrich KA, Conrad SA, Hébert CA. Cardiovascular and metabolic response to red blood cell transfusion in critically ill volume-resuscitated nonsurgical patients. Crit Care Med 1990; 18: 940-944 [Medline].
11. Babineau TJ, Dzik WH, Borlase BC, Baxter JK, Bistrian BR, Benotti PN. Reevaluation of current transfusion practices in patients in surgical intensive care units. Am J Surg 1992; 164: 22-25 [Medline].
12. Fitzgerald RD, Martin CM, Dietz GE, Doig GS, Potter RF, Sibbald WJ. Transfusing red blood cells stored in citrate phosphate dextrose adenine-1 for 28 days fails to improve tissue oxygenation in rats. Crit Care Med 1997; 25: 726-732 [Medline].
13.
Sielenkämper AW,
Chin-Yee IH,
Martin CM,
Sibbald WJ.
Diaspirin
crosslinked hemoglobin improves systemic oxygen uptake in oxygen
supply-dependent septic rats.
Am J Respir Crit Care Med
1997;
156:
1066-1072
14. Vicaut E, Stucker O, Teisseire B, Duvelleroy M. Effects of change in systemic hematocrit on the microcirculation in rat cremaster muscle. Int J Microcirc Clin Exp 1987; 6: 225-235 [Medline].
15. Lorente JA, Renes E, Gomez-Aguinaga MA, Landin L, De La Morena JL, Liste D. Oxygen delivery dependent oxygen consumption in acute respiratory failure. Crit Care Med 1991; 19: 770-775 [Medline].
16.
Karzai W,
Lötte A,
Günnicker M,
Vorgrimler-Karzai UM,
Priebe HJ.
Dobutamine increases oxygen consumption during constant flow cardiopulmonary bypass.
Br J Anaesth
1996;
76:
5-8
17. Valeri C. Viability and function of preserved red cells. N Engl J Med 1971; 284: 81-88 .
18. Haraldin AR, Weed RI, Reed CF. Changes in physical properties of stored erythrocytes. Transfusion 1969; 9: 229-235 [Medline].
19. Simchon S, Jan KM, Chien S. Influence of red cell deformability on regional blood flow. Am J Physiol 1987; 253: 895-903 .
20.
Schlichtig R,
Kramer DJ,
Pinsky MR.
Flow redistribution during progressive hemorrhage is a determinant of critical O2 delivery.
J Appl
Physiol
1991;
70:
169-178
21.
Schumacker PT,
Long GR,
Wood LDH.
Tissue oxygen extraction during hypovolemia: role of hemoglobin P50.
J Appl Physiol
1987;
62:
1801-1807
22.
Maginniss LA,
Connoly H,
Samsel RW,
Schumacker PT.
Adrenergic
vasoconstriction augments tissue O2 extraction during reductions in
O2 delivery.
J Appl Physiol
1994;
76:
1454-1461
23.
Van der Linden P,
Gilbart E,
Engelman E,
Schmartz D,
Vincent J-L.
Effects of anesthetic agents on systemic critical O2 delivery.
J Appl Physiol
1991;
71:
83-93
24.
Cain SM.
Oxygen delivery and uptake in dogs during anemic and hypoxic hypoxia.
J Appl Physiol
1977;
42:
228-234
25. Zhang H, Spapen B, Benlabed M, Vincent J-L. Systemic oxygen extraction can be increased during repeated episodes of cardiac tamponade. J Crit Care 1993; 8: 93-99 [Medline].
26.
Cain SM.
Appearance of excess lactate in anesthetized dogs during anemic and hypoxic hypoxia.
Am J Physiol
1965;
209:
604-608
27. Heusser F, Fahey JT, Lister G. Effect of hemoglobin concentration on critical cardiac output and oxygen transport. Am J Physiol 1989; 256: 527-532 .
28.
Salt PJ,
Barnes PK,
Beswick FJ.
Inhibition of neuronal and extraneuronal uptake of noradrenaline by ketamine in the isolated perfused
heart.
Br J Anaesth
1979;
51:
835-838
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