Assist in unison to the patient’s inspiratory neural effort and feedback-controlled limitation of lung distension with neurally adjusted ventilatory assist (NAVA) may reduce the negative effects of mechanical ventilation on right ventricular function.
Methods
Heart–lung interaction was evaluated in 10 intubated patients with impaired cardiac function using esophageal balloons, pulmonary artery catheters and echocardiography. Adequate NAVA level identified by a titration procedure to breathing pattern (NAVAal), 50% NAVAal, and 200% NAVAal and adequate pressure support (PSVal, defined clinically), 50% PSVal, and 150% PSVal were implemented at constant positive end-expiratory pressure for 20 minutes each.
Results
NAVAal was 3.1 ± 1.1cmH2O/μV and PSVal was 17 ± 2 cmH20. For all NAVA levels negative esophageal pressure deflections were observed during inspiration whereas this pattern was reversed during PSVal and PSVhigh. As compared to expiration, inspiratory right ventricular outflow tract velocity time integral (surrogating stroke volume) was 103 ± 4%, 109 ± 5%, and 100 ± 4% for NAVAlow, NAVAal, and NAVAhigh and 101 ± 3%, 89 ± 6%, and 83 ± 9% for PSVlow, PSVal, and PSVhigh, respectively (p < 0.001 level-mode interaction, ANOVA). Right ventricular systolic isovolumetric pressure increased from 11.0 ± 4.6 mmHg at PSVlow to 14.0 ± 4.6 mmHg at PSVhigh but remained unchanged (11.5 ± 4.7 mmHg (NAVAlow) and 10.8 ± 4.2 mmHg (NAVAhigh), level-mode interaction p = 0.005). Both indicate progressive right ventricular outflow impedance with increasing pressure support ventilation (PSV), but no change with increasing NAVA level.
Conclusions
Right ventricular performance is less impaired during NAVA compared to PSV as used in this study. Proposed mechanisms are preservation of cyclic intrathoracic pressure changes characteristic of spontaneous breathing and limitation of right-ventricular outflow impedance during inspiration, regardless of the NAVA level.
Trial registration
Clinicaltrials.gov Identifier: NCT00647361, registered 19 March 2008
Additional file 2: Shows the NAVA level titration procedure as described previously[6]-[9]. The NAVA level was reduced to a minimum of 0 cmH2O/μl resulting in delivery of 2 cmH2O (default assist level) when the inspiratory effort exceeded the pneumatic trigger threshold. When sufficient electrical activity of the diaphragm (EAdi, green tracing; middle plot) was detectable, the NAVA level (white tracing; uppermost plot) was manually increased by 0.1 cmH2O/μV every 20 seconds. By observing the airway pressure (Paw, yellow tracing; uppermost plot) and tidal volume (Vt, blue tracing; lowermost plot) on the trend screen of the ventilator monitor, NAVAal was determined as the NAVA level early after the transition from an initial steep increase in Paw and Vt (first response) to a less steep increase or even plateau in Paw and Vt (second response). NAVAlow was arbitrarily defined as 50% of NAVAal. NAVAhigh was defined as the highest level resulting in a breathing pattern similar to that observed at NAVAal (that is, before the breathing pattern became unstable and airway pressure started to increase further) [6] or at 200% of NAVAal, whatever occurred first. (PPTX 561 KB)
Additional file 6: Shows the breathing pattern and transpulmonary pressures. Left: Respiratory cycle and tidal volume for each experimental condition. PBW, predicted body weight [31]. While remaining constant under NAVA, the tidal volume increased (P < 0.001 for level*mode interaction) and the duty cycle (the inspiratory proportion total cycle time) and respiratory rate decreased (P < 0.005 and P < 0.001 respectively, level*mode interaction) with increasing the PSV level. NAVA, neurally adjusted ventilatory assist; PSV, pressure support ventilation; respective support levels, low, al (adequate level), and high. Values presented as mean ± standard deviation. Right: Transpulmonary pressure (Ptp) isobars (dotted ascending lines). Transpulmonary pressure increased from NAVAlow to NAVAal but remained stable when further increasing the assist to NAVAhigh. With PSV the transpulmonary pressure steadily increased from PSVlow to PSVhigh. Mean inspiratory airway pressure (including PEEP) and Ptp were lower during NAVA compared with the corresponding PSV levels (P < 0.05 for all, level*mode interaction). Mean inspiratory esophageal pressure deflection was negative for all NAVA levels, whereas it was negative only for PSVlow and positive for PSVal and PSVhigh (P < 0.001 for all comparisons). (PPTX 272 KB)
The online version of this article (doi:10.1186/s13054-014-0499-8) contains supplementary material, which is available to authorized users.
Competing interests
The Department of Intensive Care Medicine of University Hospital Bern has a research and development collaboration contract with Maquet Critical Care AB. None of the authors from this department received any personal financial gain from this collaboration. LB and JT were invited speakers at symposiums sponsored by Maquet Critical Care AB but did not receive any personal financial gain. DB and SB do not have any nonfinancial competing interests.
CS has patented inventions related to neural control of mechanical ventilation. The license for these patents belongs to Maquet Critical Care AB. Commercial use of this technology provides financial benefit to CS through royalties. CS owns 50% of Neurovent Research Inc., a research and development company for research studies. Neurovent Research Inc. has a consulting agreement with Maquet Critical Care AB.
Authors’ contributions
DB was involved in the development of the study protocol, conducted the study, analyzed respiratory and hemodynamic data, and made the first draft of the manuscript. SB was involved in the development of the protocol, conducted the study, performed and analyzed all echocardiography studies, and contributed to the manuscript. JT was involved in the development of the protocol, in data interpretation, and in writing the manuscript. CS was involved in the development of the study protocol, in data interpretation, and in writing the manuscript. LB designed the study and wrote the final version of the study protocol, established the experimental equipment, and was involved in data acquisition and interpretation and in writing the manuscript. LB is the guarantor of the manuscript’s content. All authors read and approved the final version of the manuscript.
Abkürzungen
CVP
central venous pressure
EAdi
electrical activity of the diaphragm
NAVA
neurally adjusted ventilator assist
NAVAal
adequate neurally adjusted ventilator assist level identified by a titration procedure
NAVAhigh
200% of the adequate neurally adjusted ventilator assist level
NAVAlow
50% of the adequate neurally adjusted ventilator assist level
PAP
pulmonary artery pressure
PEEP
positive end-expiratory pressure
Pes
esophageal pressure
PSV
pressure support ventilation
PSVal
adequate level of pressure support ventilation identified on clinical grounds
PSVhigh
150% of adequate pressure support level
PSVlow
50% of adequate pressure support level
RVOT VTI
velocity time integral in right ventricular outflow tract
Introduction
Cyclic increases in intrathoracic pressure during positive pressure ventilation may reduce venous return and increase the afterload of the right ventricle [1],[2]. Neurally adjusted ventilatory assist (NAVA) delivers inspiratory support in synchrony and in linear proportion to the neural inspiratory effort by using the electrical activity of the diaphragm (EAdi) to drive the ventilator [3]. The inspiratory muscle activity, that is synchronous and proportional to assist delivery during NAVA, is likely to attenuate the increases in pleural pressure associated with conventional positive pressure ventilation. This attenuation should reduce negative effects of positive pressure ventilation on cardiovascular function. Data on cardiovascular function during NAVA are very limited. The cardiovascular effects of NAVA depend on the pleural pressure changes and the consequent transmural vascular and cardiac pressures, but these have not so far been studied.
We hypothesized that the synchronous inspiratory muscle activity during NAVA and the feedback controlled limitation of lung volumes during increasing NAVA support avoid the adverse effects of conventional pressure support ventilation (PSV) on right ventricular afterload and venous return. We therefore compared the short-term hemodynamic effects of three NAVA and three PSV levels using simultaneous analysis of intravascular, intracardiac, esophageal pressure (Pes), airway pressure, breathing pattern, and echocardiography in patients with impaired cardiac function, chronic obstructive pulmonary disease, or both.
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Materials and methods
The Ethics Committee of Canton Bern, Switzerland approved the protocol (KEK Nr 217–06). Recruitment lasted from March to November 2010. Written informed consent from the patient’s family and deferred consent after recovery were obtained. A detailed description of the methods is provided in Additional file 1.
The main inclusion criteria were invasive mechanical ventilation, pneumatic triggering, pulmonary artery catheter monitoring for clinical reasons, and at least one of the following: left ventricular ejection fraction ≤40%; inotropic drugs (dobutamine ≥2 μg/kg/minute or adrenaline ≥0.03 μg/kg/minute); pulmonary artery occlusion pressure ≥18 mmHg; or history of chronic obstructive pulmonary disease.
Study protocol
Catheters were inserted for measurement of Pes (SmartCath; Viasys Healthcare, San Diego, CA, USA) and EAdi (Maquet, Solna, Sweden). Correct positioning of the Pes catheter was verified using an occlusion test [4],[5]. A schematic study protocol is depicted in Figure 1.
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Adequate PSV (PSVal) was set by an independent intensivist blinded for the EAdi and Pes aiming to achieve optimal patient comfort, avoid unassisted wasted inspiratory efforts, and minimize negative inspiratory deflections in central venous and pulmonary artery pressures (indicating inspiratory effort). PSVlow was 50% PSVal, and PSVhigh was 150% PSVal. Positive end-expiratory pressure (PEEP) and other prescribed ventilator settings were kept constant throughout the protocol.
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Adequate NAVA (NAVAal) was identified using a previously described titration procedure (Additional files 1 and 2[6]-[9]). NAVAlow was 50% NAVAal, and NAVAhigh was defined as the highest level sustaining a regular breathing pattern similar to that at NAVAal or 200% NAVAal, whichever occurred first.
The order of the ventilatory modes was randomized. The six ventilator settings were applied for at least 20 minutes each. All medications including sedation (Richmond agitation and sedation scale of −1 to −2 [10]) remained unchanged.
Measurements
Intravascular pressures, airway pressure, Pes, EAdi (as the percentage of EAdi without assist at the beginning of NAVA titration), and airflow were recorded continuously (Neurovent Research Inc., Toronto, ON, Canada). Pulmonary artery occlusion pressure, right ventricular pressure, and blood gases were measured at the end of each experimental period.
All signals were analyzed off-line breath by breath, using a semi-automated detection of inspiration and expiration based on airflow reversal [6]-[8]. Two approaches were used to evaluate the hemodynamic responses. First, intravascular pressure and Pes during all breaths in each ventilator setting were averaged separately during inspiration and expiration. This was done in order to include the impact of variability in breathing pattern on hemodynamics. Transmural vascular pressures were obtained by subtraction of the time integral of Pes from the respective intravascular pressure. Changes of intravascular pressures from inspiration to expiration (cyclic pressure changes) were characterized by subtracting the mean expiratory pressure from the mean inspiratory pressure (Additional file 3). The mean inspiratory Pes deflection was calculated for the duration of inspiratory airflow and was referenced to the Pes immediately preceding the start of inspiratory airflow.
Second, representative single-breath cycles were manually selected for each experimental period. The selected breaths had mean inspiratory transpulmonary pressures equal to the mean of all breaths for the specific study period (the average breath). For each of these single breaths, the central venous pressure (CVP) was measured at the base of the c wave [11]. The right ventricular isovolumetric pressure change was calculated as the difference between the base of the c wave of CVP and the pulmonary artery pressure (PAP) at valve opening [12], and the right ventricular total pressure generation was calculated as the pressure difference from the end-diastolic filling of the right ventricle (estimated as the base of the CVP c wave) to the systolic PAP. An example of this analysis is given in Additional file 4.
Pulsed wave Doppler profiles from both ventricular outflow tracts were recorded simultaneously with airway pressure during transthoracic echocardiography and were analyzed offline (Vivid 7, EchoPAC Dimension `06; GE Medical Systems, Glattbrugg, Switzerland). End-inspiratory and end-expiratory heart beats [13] from three ventilatory cycles were analyzed for each condition. To characterize the effects of lung inflation on the Doppler flow profiles, the values at end inspiration were expressed as a percentage of the values at end expiration measured during the same breathing cycle. A value >100% would thus reflect a higher value during inspiration compared with expiration, and vice versa.
Statistical analysis
Repeated-measures analysis of variance (within-subject factors: ventilation mode, support level) was used for analysis. Significant mode*support level interactions were analyzed post hoc within each mode between support levels using Sidak’s correction (IBM SPSS 20.0.0; IBM Corp, Armonk, NY, USA). Data are presented as mean ± standard deviation. P <0.05 was considered significant.
Results
Ten patients (age 66 ± 10 years; five females; Simplified Acute Physiology Score II 41 ± 9) were studied (Table 1). Figure 2 illustrates the respiratory pattern and cyclic intravascular pressure changes for all experimental conditions in a single patient.
Table 1
Characteristics of individual patients
Patient number
PBW (kg)
BMI (kg/m2)
SAPS II
ICU LOS (days)
Perioperative LVEF (%)
Prestudy PAOP (mmHg)
Prestudy cardiac index (l/minute/m2)
Dobutamine during study (μg/kg/minute)
Cardiopulmonary diagnosis
1
72
26
42
1.8
35
15
1.4
3.1
CABG
2
60
24
34
0.9
31
14
2.6
3.8
CABG
3
57
30
37
1.0
40
12
3.2
0.0
CABG, COPD with cor pulmonale
4
50
31
35
0.9
35
8
1.6
3.4
CABG, aortic valve replacement
5
73
31
54
3.4
35
13
3.6
0.0
Cardiogenic shock following myocardial infarction
6
52
23
40
0.9
30
13
2.2
4.5
CABG, aortic valve replacement, COPD
7
53
34
26
3.7
65
17
2.2
2.9
Aortic valve and arch replacement (type A dissection)
8
73
34
37
3.8
36
16
2.8
0.0
Aortic and mitral valve replacement, COPD
9
64
30
57
6.9
30
11
3.0
3.9
CABG, aortic valve replacement, mitral ring
10
69
24
44
19.8
25
26
3.1
0.0
Cardiogenic shock following myocardial infarction
BMI, body mass index; CABG, coronary artery bypass graft; COPD, chronic obstructive pulmonary disease; LOS, length of stay; LVEF, left ventricular ejection fraction; PAOP, pulmonary artery occlusion pressure; PBW, predicted body weight; SAPS, Simplified Acute Physiology Score.
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Five patients with reduced left ventricular ejection fraction and one patient with normal left ventricular ejection fraction (Patient 7) received inotropic drug support (dobutamine, mean dose 2.2 ± 1.9 μg/kg/minute), and four patients with reduced left ventricular ejection fraction did not receive inotropic medication. Biological valves were used for all valve surgery procedures.
NAVAal was identified at 3.1 ± 1.1 cmH2O/μV and PSVal at 17 ± 2 cmH2O, with a PEEP of 7 ± 2 cmH2O (Additional file 5). EAdi was lower with PSV than with NAVA. The tidal volume and transpulmonary pressure increased from NAVAlow to NAVAal and did not increase further at NAVAhigh, whereas both parameters increased with increasing PSV (Table 2 and Additional file 6). Table 2 presents data on the respiratory pattern and the systemic hemodynamic function.
Table 2
Blood gases, respiratory pattern and systemic hemodynamic data
PSVlow
PSVal
PSVhigh
NAVAlow
NAVAal
NAVAhigh
P value
Level
Mode
Interaction
Blood gases
PaO2 (mmHg)
94 ± 21
94 ± 21
97 ± 21
94 ± 25
91 ± 25
94 ± 24
0.325
0.495
0.864
PaCO2 (mmHg)
38 ± 9
37 ± 8
36 ± 8
39 ± 10
39 ± 11
38 ± 9
<0.001
0.202
0.102
SaO2 (%)
97 ± 2
97 ± 1
98 ± 2
97 ± 2
97 ± 2
97 ± 2
0.174
0.309
0.782
pH
7.41 ± 0.1
7.43 ± 0.1
7.45 ± 0.1
7.42 ± 0.1
7.43 ± 0.1
7.43 ± 0.1
<0.001
0.464
0.164
Base excess
0.2 ± 3.6
0.3 ± 3.6
0.1 ± 3.6
0.4 ± 3.5
0.5 ± 3.5
0.5 ± 3.5
0.194
0.244
0.592
Respiratory pattern
Respiratory rate (breaths/minute)
21 ± 5
18 ± 4
13 ± 3
20 ± 5
21 ± 5
20 ± 6
<0.001
0.041
<0.001
Tidal volume (ml/kg PBW)
6.3 ± 1.1
8.2 ± 1.8
11.4 ± 3.0
6.7 ± 1.2
7.0 ± 1.2
7.6 ± 1.2
<0.001
0.018
0.001
Minute ventilation (l/minute)
7.7 ± 2.0
8.6 ± 2.5
8.7 ± 2.1
8.1 ± 2.7
8.6 ± 2.5
8.7 ± 3.0
<0.001
0.619
0.361
Electrical activity of the diaphragm (% EAdi max)
61 ± 16
32 ± 11
17 ± 9
90 ± 33
71 ± 19
29 ± 25
<0.001
0.002
0.3
Mean inspiratory transpulmonary pressure (cmH2O)
3 ± 4
5 ± 4
10 ± 4
3 ± 3
3 ± 4
7 ± 5
<0.001
0.158
<0.001
Mean esophageal pressure deflection (cmH2O)
−0.7 ± 1.5
2.1 ± 1.9
4 ± 2.3
−1.5 ± 2.4
−1.5 ± 1.7
0 ± 1
0.001
<0.001
<0.001
Systemic hemodynamic data
Pulmonary artery occlusion pressure (mmHg)
16 ± 7
14 ± 4
15 ± 7
15 ± 7
15 ± 5
16 ± 6
0.516
0.424
0.241
Mean systemic arterial pressure (mmHg)
65 ± 8
61 ± 9
65 ± 9
65 ± 9
63 ± 9
63 ± 9
0.065
0.922
0.256
Heart rate (beats/minute)
90 ± 9
90 ± 9
89 ± 9
89 ± 10
90 ± 10
88 ± 10
0.3
0.831
0.567
Cardiac output (l/minute)
4.7 ± 0.9
4.8 ± 0.7
4.8 ± 0.7
5.2 ± 1.2
5.1 ± 1.1
5.1 ± 1.2
0.964
0.082
0.284
Mixed venous oxygen saturation (%)
66 ± 7
64 ± 5
66 ± 9
63 ± 5
65 ± 7
62 ± 5
0.469
0.059
0.211
Data presented as mean ± standard deviation. P values from repeated-measures analysis of variance (within-subject factors: ventilation mode, support level). NAVA, neurally adjusted ventilator assist; NAVAal, adequate NAVA level identified by a titration procedure; NAVAhigh, 200% of the adequate NAVA level; NAVAlow, 50% of the adequate NAVA level; PaCO2, partial pressure of carbon dioxide; PaO2, partial pressure of oxygen; PBW, predicted body weight; PSV, pressure support ventilation; PSVal, adequate level of pressure support ventilation identified on clinical grounds; PSVhigh, 150% of adequate PSV level; PSVlow, 50% of adequate PSV level; SaO2, oxygen saturation in arterial blood.
Transmural pressures
There was no difference between the modes in intravascular or transmural CVP and PAP in expiration. The cyclic changes (inspiratory minus expiratory values) in transmural CVP were small with both NAVA and PSV, and decreased with increasing level of support more prominently with PSV (P = 0.03, level*mode interaction). The cyclic changes in transmural PAP were negative for all NAVA levels and PSVlow, and were positive for PSVal and PSVhigh (P = 0.026, level*mode interaction; Table 3). The inspiratory deflections in Pes became progressively positive with increasing PSV, while they remained negative with all NAVA levels (P < 0.001, level*mode interaction).
Table 3
Mean central venous and mean pulmonary artery pressures for the entire experimental period
PSVlow
PSVal
PSVhigh
NAVAlow
NAVAal
NAVAhigh
P value
Level
Mode
Interaction
Expiratory values
Central venous pressure (mmHg)
10 ± 3
10 ± 3
10 ± 3
11 ± 3
10 ± 3
11 ± 3
0.064
0.091
0.919
Mean pulmonary artery pressure (mmHg)
30 ± 8
27 ± 6
27 ± 6
30 ± 5
29 ± 5
28 ± 5
0.002
0.065
0.208
Transmural central venous pressure (mmHg)
3 ± 4
1 ± 5
2 ± 4
5 ± 4
2 ± 3
3 ± 3
0.06
0.267
0.566
Transmural mean pulmonary artery pressure (mmHg)
22 ± 9
18 ± 8
19 ± 7
24 ± 6
21 ± 5
21 ± 6
<0.001
0.091
0.683
Cyclic pressure changes
Central venous pressure (mmHg)
−0.5 ± 0.4
0.4 ± 0.4
1.0 ± 0.4
−1 ± 0.5
−0.8 ± 0.6
−0.5 ± 0.7
<0.001
<0.001
<0.001
Mean pulmonary artery pressure (mmHg)
−2.2 ± 1.1
0.5 ± 1.4
2.5 ± 1.3
−3.2 ± 0.9
−2.7 ± 1.2
−1.9 ± 1
<0.001
<0.001
<0.001
Transmural central venous pressure (mmHg)
1.3 ± 1.6
0 ± 0.9
−0.9 ± 1.1
1.4 ± 2.4
1.6 ± 1.6
0.1 ± 1.8
0.009
0.08
0.03
Transmural mean pulmonary artery pressure (mmHg)
−0.3 ± 1.8
0.1 ± 0.8
0.5 ± 0.8
−0.8 ± 2.1
−0.4 ± 1.3
−1.2 ± 1.9
0.479
0.078
0.026
Data presented as mean ± standard deviation. Central venous and pulmonary artery pressures (zeroed to atmosphere) and their respective transmural values for the different experimental periods. The transmural values were calculated by subtraction of the esophageal pressure. Cyclic pressure changes are the differences between mean inspiratory and mean expiratory pressures. Data reflect mean values from the analysis of the entire experimental periods. P values from repeated-measures analysis of variance (within-subject factors: ventilation mode, support level). NAVA, neurally adjusted ventilator assist; NAVAal, adequate NAVA level identified by a titration procedure; NAVAhigh, 200% of the adequate NAVA level; NAVAlow, 50% of the adequate NAVA level; PSV, pressure support ventilation; PSVal, adequate level of pressure support ventilation identified on clinical grounds; PSVhigh, 150% of adequate PSV level; PSVlow, 50% of adequate PSV level.
In the analysis of the representative single breath (Figure 3, Table 4), the cyclic changes in transmural CVP decreased with increasing support with both NAVA and PSV (level effect P = 0.015). The transmural CVP was higher in inspiration than in expiration at all NAVA levels, whereas increasing PSV resulted in higher CVP during expiration than during inspiration (mode effect P = 0.015).
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Table 4
Loading conditions of the right ventricle in the average breath
Cyclic change in transmural isovolumetric pressure (mmHg)
−1.8 ± 1.4
0.8 ± 2.2
2 ± 2
−1.3 ± 1
−1.8 ± 2.1
−1.3 ± 1.1
0.003
0.009
0.003
Total pressure generation
Inspiratory transmural pressure generation (mmHg)
29.7 ± 10.7
27.2 ± 7.8
29.6 ± 9.4
29.8 ± 9.6
26.9 ± 8.5
26.9 ± 7
0.06
0.38
0.561
Expiratory transmural pressure generation (mmHg)
30.4 ± 10.8
23.5 ± 8.3
26.5 ± 9.4
28.6 ± 10.4
27.9 ± 8
27 ± 6.9
0.231
0.053
0.241
Cyclic change in transmural pressure generation (mmHg)
−0.7 ± 2.3
3.8 ± 8
3.1 ± 1.5
1.2 ± 3.7
−1 ± 4.5
0 ± 2
0.543
0.076
0.033
Data presented as mean ± standard deviation. Data derived from the analysis of the single average breath with measurement of the central venous pressure (CVP) at the base of the c wave. Isovolumetric pressure generation was calculated as the difference between pulmonary artery pressure at valve opening and CVP at the c wave, and the total pressure generation as systolic pulmonary artery pressure minus CVP at the c wave. P values from repeated-measures analysis of variance (within-subject factors: ventilation mode, support level). NAVA, neurally adjusted ventilator assist; NAVAal, adequate NAVA level identified by a titration procedure; NAVAhigh, 200% of the adequate NAVA level; NAVAlow, 50% of the adequate NAVA level; PSV, pressure support ventilation; PSVal, adequate level of pressure support ventilation identified on clinical grounds; PSVhigh, 150% of adequate PSV level; PSVlow, 50% of adequate PSV level.
Right ventricular ejection
The transmural inspiratory isovolumetric pressure change increased with increasing pressure support, whereas it remained unchanged with increasing NAVA levels (P = 0.005, level*mode interaction; Table 4). Accordingly, the cyclic alterations (inspiratory minus expiratory values) in the isovolumetric pressure change increased with increasing pressure support and remained unchanged with NAVA (P = 0.003, level*mode interaction; Figure 3). A similar pattern was observed for the cyclic changes in the total transmural pressure generation of the right ventricle from central venous end diastolic pressure to systolic pulmonary artery pressure (P = 0.033, level*mode interaction).
Both the ventilation mode and support level modified the right ventricular Doppler flow patterns (Table 5, Figure 4). During inspiration the flow period and the velocity time integral in the right ventricular outflow tract (RVOT VTI, a surrogate of stroke volume) both progressively decreased with increasing PSV level, whereas they remained unchanged with increasing NAVA levels (P = 0.028 for flow period and P = 0.025 for RVOT VTI, level*mode interaction).
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Table 5
Right ventricular echocardiographic data
Doppler flow profile in the right ventricular outflow tract (n = 8)
PSVlow
PSVal
PSVhigh
NAVAlow
NAVAal
NAVAhigh
P value
Level
Mode
Interaction
End expiration
Acceleration time (milliseconds)
82 ± 14
83 ± 13
80 ± 11
82 ± 16
77 ± 14
89 ± 18
0.484
0.68
0.141
Flow period (milliseconds)
242 ± 25
256 ± 36
256 ± 37
240 ± 23
242 ± 27
243 ± 28
0.072
0.127
0.285
Maximum flow velocity (m/second)
0.8 ± 0.2
0.9 ± 0.3
0.8 ± 0.3
0.7 ± 0.3
0.8 ± 0.2
0.9 ± 0.3
0.047
0.012
0.465
Velocity time integral (cm)
13 ± 2
14 ± 3
14 ± 3
13 ± 2
13 ± 3
14 ± 3
0.009
0.063
0.178
End inspiration
Acceleration time (milliseconds)
86 ± 15
81 ± 15
84 ± 17
81 ± 12
88 ± 20
91 ± 17
0.62
0.259
0.296
Flow period (milliseconds)
250 ± 27
242 ± 25
231 ± 33
250 ± 21
261 ± 29
251 ± 30
0.02
0.067
0.028
Maximum flow velocity (m/second)
0.8 ± 0.2
0.8 ± 0.3
0.7 ± 0.2
0.7 ± 0.3
0.9 ± 0.3
0.8 ± 0.3
0.168
0.154
0.166
Velocity time integral (cm)
13 ± 3
13 ± 3
12 ± 3
13 ± 2
14 ± 3
14 ± 3
0.154
0.046
0.025
Inspiratory values as percentage of expiratory values
cAcceleration time (%)
104 ± 8
98 ± 8
105 ± 10
101 ± 13
115 ± 9
104 ± 11
0.617
0.217
0.012
Flow period (%)
103 ± 2
94 ± 3
91 ± 2
104 ± 2
107 ± 3
103 ± 2
<0.001
<0.001
<0.001
Maximum flow velocity (%)
99 ± 2
92 ± 7
86 ± 8
100 ± 3
106 ± 5
97 ± 4
<0.001
0.003
<0.001
Velocity time integral (%)
101 ± 3
89 ± 6
83 ± 9
103 ± 4
109 ± 5
100 ± 4
<0.001
<0.001
<0.001
Data presented as mean ± standard deviation. Doppler flow profiles in the right ventricular outflow tract could be obtained from eight patients. Absolute values at end expiration did not differ between NAVA and PSV. To describe cyclic changes, the inspiratory values are given as a percentage of the corresponding expiratory value. P values from repeated-measures analysis of variance (within-subject factors: ventilation mode, support level). NAVA, neurally adjusted ventilator assist; NAVAal, adequate NAVA level identified by a titration procedure; NAVAhigh, 200% of the adequate NAVA level; NAVAlow, 50% of the adequate NAVA level; PSV, pressure support ventilation; PSVal, adequate level of pressure support ventilation identified on clinical grounds; PSVhigh, 150% of adequate PSV level; PSVlow, 50% of adequate PSV level.
RVOT VTI was equal or higher during inspiration compared with expiration for all NAVA levels. With PSV, RVOT VTI was equal during inspiration and expiration only with PSVlow but it was clearly lower during inspiration compared with expiration with PSVal and PSVhigh (P < 0.001, level*mode interaction). The highest RVOT VTI during inspiration compared with expiration was observed with NAVAal (109 ± 5%). The right ventricular stroke volume, as reflected by the RVOT VTI, during inspiration was thus preserved with all NAVA levels whereas it progressively decreased with increasing PSV level.
The left ventricular echocardiography results are summarized in Additional file 7. No relevant differences were observed between the modes.
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Discussion
The main finding of this study was that ventilation with NAVA in patients with impaired cardiac function but stable hemodynamics avoided an inspiratory increase in right ventricular outflow impedance by preserving the cyclic, negative deflections in intrathoracic pressure via feedback control of transpulmonary pressure and tidal volume. The hemodynamic pattern during NAVA closely resembled that of unassisted spontaneous breathing, regardless of the NAVA level used. In contrast, increased inspiratory assist with PSV progressively increased right ventricular outflow impedance, transpulmonary pressure, and tidal volume.
The pattern of decreasing right and increasing left ventricular stroke volume during inspiration is the characteristic pattern of heart–lung interactions during positive pressure ventilation [13]-[16]. The mechanisms of stroke volume variation during the breathing cycle include changes in venous return and consequent ventricular filling [17]-[19], and changes in outflow impedance [2],[12]. Although these mechanisms have been known for decades, their implications and relevance during NAVA have not been addressed. Specifically, the actual pleural and transmural pressure profiles resulting from clinical application of NAVA will define the cardiac effects of NAVA. These have not been described before. In this respect, our study provides mechanistic insight into the heart–lung interactions of NAVA in a clinically relevant and realistic setting. We used RVOT VTI as a surrogate for right ventricular stroke volume assuming that the pulmonary valve annulus area does not vary with respiration [2]. The progressive reduction in inspiratory RVOT VTI, flow period and maximum flow velocity, and inspiratory increases in right ventricular isovolumetric contraction pressure with increasing PSV indicate increased impedance to right ventricular outflow [12]. In contrast, during all NAVA levels, right ventricular outflow impedance was lower during inspiration than during expiration, as indicated by increased inspiratory RVOT VTI, flow period and maximum flow velocity and reduced right ventricular isovolumetric contraction pressure. Reduced right ventricular afterload during inspiration with NAVA and increased inspiratory afterload with PSV is further supported by negative correlation between inspiratory changes in RVOT VTI and Pes (reflecting pleural pressure; Figure 4) and the decreased RVOT VTI with increased pressures in the pressure/flow diagrams (Additional file 8) [20].
Reduced right ventricular preload due to positive pressure ventilation-associated reduction in venous return [17],[19],[21] was also likely to contribute to changes in RVOT VTI. Since we did not measure pericardial pressure, we have no direct estimates of right ventricular end-diastolic wall tension. The transmural pressure at the base of the c wave of the CVP tracing, a surrogate of right ventricular end-diastolic wall tension, decreased slightly but significantly with increasing support both in inspiration and expiration without difference between modes. This result should be interpreted with caution, since pleural pressure may not adequately reflect pericardial pressure [22]. Nevertheless, even if changes in preload were involved, the increased right ventricular isovolumetric contraction pressure in the presence of reduced RVOT VTI indicates increased impedance to right ventricular ejection [12] in inspiration with PSV, and the opposite changes indicate reduced impedance to ejection during inspiration with NAVA. The increase in the right ventricle afterload has been assumed to be relevant mainly at high lung volumes [23]-[25]. Our results clearly indicate the presence of this mechanism also at low tidal volumes, although it did not compromise cardiac performance in our patients with stable hemodynamics to a clinically relevant extent.
Mean inspiratory Pes deflection increased progressively with increasing PSV, whereas the initially slightly negative Pes deflection approached zero with increasing NAVA levels, but did not increase further. This may be related to a progressive downregulation of EAdi with increasing NAVA level, and might limit the effect of NAVA on right ventricular function. Such feedback mechanisms have been previously observed in healthy volunteers and mechanically ventilated patients with acute respiratory failure [6]-[8],[26].
Study limitations
Several limitations must be addressed. The study was carried out to demonstrate the underlying physiology; due to safety concerns, patients with impaired cardiac function but stable hemodynamic and metabolic conditions were studied for short periods only. Hence, the relevance and consequences of treatment, if any, of these potentially beneficial effects of NAVA should be evaluated further in hemodynamically unstable patients with compromised right ventricular function and in patients with deranged metabolic conditions or with hypercapnia or hypoxemia – clinical conditions where substantial unloading of respiratory muscles with minimum compromise of right ventricular function may be considered.
Most of the patients were studied during the first day after cardiac surgery. Despite being clinically stable, some of these patients could have had relevant intravascular volume changes. In fact, hypovolemia is known to aggravate cyclic intravascular pressure swings [27]-[29]. Despite potential differences in preload status, the observed hemodynamic response seem consistent within and among individual patients.
There is no standard approach to titrate NAVA. We previously used the same NAVAal titration for several days in ICU patients with critical illness associated polyneuromyopathy (CIPM) without progression to respiratory distress, suggesting that NAVAal provides sufficient respiratory support [8].The average PSV adjusted by the clinicians in charge was based on clinical evaluation of patient comfort, and as a substitute for inspiratory effort, to minimize the cyclic changes in intrathoracic intravascular pressures. The resulting relatively high PSV can be criticized for augmenting the effects of PSV on right ventricular function. However, most patients were likely to have reduced chest wall compliance due to obesity and recent cardiac surgery. The average level of PSV also coincided with the reported average level associated with best patient comfort in difficult to wean patients [30]. PEEP may influence respiratory drive and assist requirements [7], but PEEP was kept constant and should not have influenced the changes within patients. Finally, since PSV and NAVA result in different flow patterns and as flow reversal was used to identify the transition between inspiration and expiration, the investigators could not be blinded to the mode used when analyzing the data.
Conclusions
In patients with impaired cardiac function, right ventricular performance is less impaired during NAVA titrated to the breathing pattern compared with PSV selected based on clinical criteria. Proposed mechanisms are preservation of cyclic intrathoracic pressure changes characteristic of spontaneous breathing and limitation of right-ventricular outflow impedance during inspiration, regardless of the NAVA level. Thus, NAVA not only prevents lung overdistension and potentially diaphragm disuse, but also the characteristic side effects of positive pressure ventilation on right ventricular function.
Key messages
During NAVA, a ventilatory mode that delivers assist in proportion to the neural inspiratory effort, the right-ventricular hemodynamic pattern resembles that of unassisted spontaneous breathing, regardless of the NAVA level used.
The proposed mechanism includes a lack of increase in right ventricular outflow impedance and a lack of decrease in venous return during lung inflation.
During NAVA, lung inflation and tidal volume are restricted by neural feedback, while near-zero negative deflections in intrathoracic pressure are preserved.
Authors’ information
DB and SB share the position of first author.
Additional files
Acknowledgments
The authors are indebted to the study patients for their participation, to Norman Comtois for his excellent technical assistance, to Jennifer Beck for the expert review of the manuscript, and to the study nurses from our institution, especially Michael Lensch, for their assistance with the experimental setup. The authors thank the physicians and the nursing staff of the Department of Intensive Care Medicine, Bern University Hospital (Inselspital) for their valuable cooperation. The study was supported by a grant from the Swiss National Science Foundation (SNF) 3200B0-113478/1 and from the Stiftung für die Forschung in Anästhesiologie und Intensivmedizin (Foundation for Research in Anesthesiology and Intensive Care), Bern (18/2006) awarded to LB.
Competing interests
The Department of Intensive Care Medicine of University Hospital Bern has a research and development collaboration contract with Maquet Critical Care AB. None of the authors from this department received any personal financial gain from this collaboration. LB and JT were invited speakers at symposiums sponsored by Maquet Critical Care AB but did not receive any personal financial gain. DB and SB do not have any nonfinancial competing interests.
CS has patented inventions related to neural control of mechanical ventilation. The license for these patents belongs to Maquet Critical Care AB. Commercial use of this technology provides financial benefit to CS through royalties. CS owns 50% of Neurovent Research Inc., a research and development company for research studies. Neurovent Research Inc. has a consulting agreement with Maquet Critical Care AB.
Authors’ contributions
DB was involved in the development of the study protocol, conducted the study, analyzed respiratory and hemodynamic data, and made the first draft of the manuscript. SB was involved in the development of the protocol, conducted the study, performed and analyzed all echocardiography studies, and contributed to the manuscript. JT was involved in the development of the protocol, in data interpretation, and in writing the manuscript. CS was involved in the development of the study protocol, in data interpretation, and in writing the manuscript. LB designed the study and wrote the final version of the study protocol, established the experimental equipment, and was involved in data acquisition and interpretation and in writing the manuscript. LB is the guarantor of the manuscript’s content. All authors read and approved the final version of the manuscript.
Additional file 2: Shows the NAVA level titration procedure as described previously[6]-[9]. The NAVA level was reduced to a minimum of 0 cmH2O/μl resulting in delivery of 2 cmH2O (default assist level) when the inspiratory effort exceeded the pneumatic trigger threshold. When sufficient electrical activity of the diaphragm (EAdi, green tracing; middle plot) was detectable, the NAVA level (white tracing; uppermost plot) was manually increased by 0.1 cmH2O/μV every 20 seconds. By observing the airway pressure (Paw, yellow tracing; uppermost plot) and tidal volume (Vt, blue tracing; lowermost plot) on the trend screen of the ventilator monitor, NAVAal was determined as the NAVA level early after the transition from an initial steep increase in Paw and Vt (first response) to a less steep increase or even plateau in Paw and Vt (second response). NAVAlow was arbitrarily defined as 50% of NAVAal. NAVAhigh was defined as the highest level resulting in a breathing pattern similar to that observed at NAVAal (that is, before the breathing pattern became unstable and airway pressure started to increase further) [6] or at 200% of NAVAal, whatever occurred first. (PPTX 561 KB)
Additional file 6: Shows the breathing pattern and transpulmonary pressures. Left: Respiratory cycle and tidal volume for each experimental condition. PBW, predicted body weight [31]. While remaining constant under NAVA, the tidal volume increased (P < 0.001 for level*mode interaction) and the duty cycle (the inspiratory proportion total cycle time) and respiratory rate decreased (P < 0.005 and P < 0.001 respectively, level*mode interaction) with increasing the PSV level. NAVA, neurally adjusted ventilatory assist; PSV, pressure support ventilation; respective support levels, low, al (adequate level), and high. Values presented as mean ± standard deviation. Right: Transpulmonary pressure (Ptp) isobars (dotted ascending lines). Transpulmonary pressure increased from NAVAlow to NAVAal but remained stable when further increasing the assist to NAVAhigh. With PSV the transpulmonary pressure steadily increased from PSVlow to PSVhigh. Mean inspiratory airway pressure (including PEEP) and Ptp were lower during NAVA compared with the corresponding PSV levels (P < 0.05 for all, level*mode interaction). Mean inspiratory esophageal pressure deflection was negative for all NAVA levels, whereas it was negative only for PSVlow and positive for PSVal and PSVhigh (P < 0.001 for all comparisons). (PPTX 272 KB)