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Erschienen in: BMC Anesthesiology 1/2015

Open Access 01.12.2015 | Research article

Accuracy of an autocalibrated pulse contour analysis in cardiac surgery patients: a bi-center clinical trial

verfasst von: Ole Broch, Jose Carbonell, Carlos Ferrando, Malte Metzner, Arne Carstens, Martin Albrecht, Matthias Gruenewald, Jan Höcker, Marina Soro, Markus Steinfath, Jochen Renner, Berthold Bein

Erschienen in: BMC Anesthesiology | Ausgabe 1/2015

Abstract

Background

Less-invasive and easy to install monitoring systems for continuous estimation of cardiac index (CI) have gained increasing interest, especially in cardiac surgery patients who often exhibit abrupt haemodynamic changes. The aim of the present study was to compare the accuracy of CI by a new semi-invasive monitoring system with transpulmonary thermodilution before and after cardiopulmonary bypass (CPB).

Methods

Sixty-five patients (41 Germany, 24 Spain) scheduled for elective coronary surgery were studied before and after CPB, respectively. Measurements included CI obtained by transpulmonary thermodilution (CITPTD) and autocalibrated semi-invasive pulse contour analysis (CIPFX). Percentage changes of CI were also calculated.

Results

There was only a poor correlation between CITPTD and CIPFX both before (r 2 = 0.34, p < 0.0001) and after (r 2 = 0.31, p < 0.0001) CPB, with a percentage error (PE) of 62 and 49 %, respectively. Four quadrant plots revealed a concordance rate over 90 % indicating an acceptable correlation of trends between CITPTD and CIPFX before (concordance: 93 %) and after (concordance: 94 %) CPB. In contrast, polar plot analysis showed poor trending before and an acceptable trending ability of changes in CI after CPB.

Conclusions

Semi-invasive CI by autocalibrated pulse contour analysis showed a poor ability to estimate CI compared with transpulmonary thermodilution. Furthermore, the new semi-invasive device revealed an acceptable trending ability for haemodynamic changes only after CPB.

Trial registration

ClinicalTrials.gov: NCT02312505 Date: 12.03.2012
Hinweise
Jochen Renner and Berthold Bein contributed equally to this work.

Competing interests

Dr. Bein is a member of the medical advisory board of Pulsion Medical Systems (Munich, Germany) and has received honoraria for consulting and giving lectures.
Dr. Renner has received honoraria from Edwards Lifesciences (Irvine, CA, USA) for giving lectures.
Dr. Gruenewald has received honoraria from GE Healthcare (Munich, Germany) for giving lectures. All other authors declare no competing interests.

Authors’ contributions

OB conducted the study, analyzed the data and drafted the manuscript. JC and CF conducted the study. MM and AC has made substantial contributions to data acquisition and has been involved in drafting the manuscript. MA and MG participated in statistical analysis and helped to draft the manuscript. JH has made contributions to data analysis and study design. MSo participated in data analysis and coordination of the study. MSt has been involved in drafting the manuscript and participated in study design. JR participated in study design and coordination and helped to draft the manuscript. BB conceived of the study, helped with drafting the manuscript and data analysis. All authors read and approved the final manuscript.

Authors` information

OB works as a consultant at the Department for Anaesthesiology and Intensive Care Medicine, University Hospital Schleswig-Holstein, Campus Kiel. His clinical focus area is anaesthesia in cardiac surgery and paediatric cardiac surgery. Research interests are haemodynamic monitoring, fluid therapy and patient outcome.

Background

Most of the studies applying algorithms for haemodynamic optimization of high-risk surgical patients have used cardiac index (CI) as one important target. Furthermore, these investigations could demonstrate that optimization of CI was associated with a significant lower rate of postoperative morbidity and mortality [1]. In the past, estimation of CI was mostly performed by pulmonary or transpulmonary thermodilution (TPTD) which due to their invasiveness are associated with considerable complications [24]. Therefore, interest has focused on less-invasive, readily available and easy to install techniques which are based for example on continuous arterial waveform analysis [57]. By using established arterial catheters, pulse contour analysis offers the opportunity for continuous estimation of CI and other haemodynamic variables like systemic vascular resistance or stroke volume variation, enabling the clinician to respond quickly and effectively to abrupt haemodynamic changes. The recently introduced semi-invasive monitoring system PulsioFlex (Pulsion Medical Systems, Munich, Germany) was developed for continuous CI trending and consists of an algorithm that provides beat-to-beat estimation of CI by analysis of the arterial blood pressure tracing. By using a proprietary “autocalibration” mode this software also calculates the individual aortic compliance and systemic vascular resistance based on patient data such as age, height, weight and gender.
The aim of the present study was to investigate accuracy and trending ability of the autocalibrated semi-invasive CI (CIPFX) with transpulmonary thermodilution (CITPTD) before and after cardiopulmonary bypass (CPB).

Methods

This study was conducted in compliance with the Helsinki declaration. After approval from institutional ethics committee (Ethikkomission UKSH Kiel - AZ 162/10, Christian-Albrechts-University Kiel, Schwanenweg 20, D 24105 Kiel; Comite Etico de Investigación Clinica, Hospital Clinico Universitario, Blasco Ibanez 17, Valencia 46010 Spain), written informed consent for participation in the study was obtained preoperatively from all patients. The trial was registered on ClinicalTrials.gov (NCT02312505). Sixty-five patients (41 patients Germany, 24 patients Spain) undergoing elective coronary artery bypass grafting (CABG) were studied after induction of general anaesthesia until discharge to the intensive care unit. Exclusion criteria were patients less than 18 years of age, a left ventricular ejection fraction ≤0.5, a lack of sinus rhythm, valvular heart diseases, emergency procedures and patients requiring mechanical support or continuous high-dose (>0.1 μg/kg/min) catecholamine therapy.

Study protocol

All patients received midazolam 0.1 mg/kg orally 30 minutes before induction of anaesthesia. After establishment of monitoring of peripheral oxygen saturation (SpO2) and heart rate (HR) patients received a peripheral venous access and a radial arterial line in Seldinger-technique (Arrow International, Inc. Reading, PA, USA). According to the manufacturer’s instructions, a PulsioFlex system (Pulsion Medical Systems, Munich, Germany) was connected to the arterial line. Adjustment of the transducer was followed by zeroing and input of individual demographic data. Thereafter, autocalibration of the semi-invasive device was performed. All variables were automatically indexed to body surface area.
After induction of anaesthesia, a central venous catheter and a transpulmonary thermodilution catheter (Pulsion Medical Systems, Munich, Germany) were introduced in the right internal jugular vein and in the femoral artery, respectively. Patients were ventilated with the ADU S5 ventilator (Datex Ohmeda, GE Healthcare, Munich, Germany) in a volume-controlled mode with a tidal volume of 6–8 ml/kg, a positive end-expiratory pressure of 5 cm H2O, an I:E ratio of 1:1.5 and a FiO2 of 0.5. Respiratory rate was adjusted to achieve normocapnia (pCO2 35–40 mmHg) and end-tidal carbon dioxid was measured with an infrared absorption analyzer. The thermodilution catheter was connected to the PiCCO2 monitor (Software version 1.3.0.8). The passive leg raising manoeuvre (PLR) was performed by a leg elevation up to 45° with the trunk in the horizontal position, inducing haemodynamic changes by transferring blood towards the central compartment.

Data collection

After induction of anaesthesia and establishment of all monitoring devices including autocalibration of the semi-invasive device, a PLR was performed and haemodynamic variables including CI (CITPTD, CIPFX) and stroke volume index (SVI) were recorded before, during and after PLR. Subsequently, estimation of CITPTD and CIPFX were carried out every 10 minutes until the beginning of CPB (T1). Number of measurements differed from patient to patient, depending on the experience of the surgeon and time needed for preparation. Stable haemodynamic conditions and exclusion of an under- or overdamped arterial signal were prerequisites for the measurements. Estimation of CITPTD was based on injecting 15 ml ice cold saline (≤8°C) at least three times through the central venous line. Measurements were repeated if CI between individual measurements differed ≥15 %. Estimation of CIPFX was performed simultaneously by recording and averaging five values over a period of two minutes. In case of a difference ≥15 % values of CIPFX were also discarded. Fifteen minutes after weaning from CPB, autocalibration of the semi-invasive monitoring system was performed again and estimation of CITPTD and CIPFX was restarted up to the end of the surgical intervention (T2). Again, due to different time needed for surgery, a different number of measurement pairs in individual patients were obtained during this time period (Fig. 1). There was no deviation from the study protocol.

Statistical analysis

Statistical comparisons were performed using commercially available statistics software (GraphPad Prism 5, GraphPad Software Inc., San Diego, CA, USA; MedCalc for Windows, version 11.6.1.0, MedCalc Software, Mariakerke, Belgium; SigmaPlot 13.0 for Windows version 7, Systat Software, Inc., San Jose, CA). For demonstration of the relationship between sample size and the width of the confidence interval of the estimated variable, we calculated the width of the 95 % confidence interval of the limits of agreement (as \( \pm 1.96\sqrt{\frac{3}{n}}\cdot s \), where s is the standard deviation of the bias) as recommended by Bland and Altman [8]. All data are given as mean ± SD and a p value <0.05 was considered significant. Linear correlations between the measurements of CITPTD and CIPFX were calculated. To plot the agreement between CITPTD and CIPFX, a Bland-Altman analysis for repeated measurements was performed for each time period (T1-T2). We used the limits of agreement (2SD) of the bias divided by the mean CI values from CITPTD and CIPFX for calculation of the percentage error and determined a 30 % threshold as previously described by Critchley and colleagues [9]. As suggested by a recent literature, we described the trending ability using different statistical techniques [10, 11]. Trending ability was assessed by determination of correlation coefficients between ∆CITPTD and ∆CIPFX, by a modified Bland-Altman analysis using the change in CI between sequential readings, a four quadrant analysis and polar plots. The concordance in the direction of change between ∆CITPTD and ∆CIPFX was estimated. Changes of CITPTD < 15 % were excluded from analysis and a concordance rate of >90 % was considered reflecting a reliable trending ability as recommended by Critchley and colleagues [11]. The distance from the center of the polar plots reflects the mean change in CI. The angle ϴ with the horizontal axis represents agreement between the ∆CI value and reference technique (∆CITPTD). The higher the agreement, the closer data pairs will lie along the radial axis. If ϴ equals 0°, the agreement between both ∆CI values is 100 %, but if ϴ is 90° there is no agreement at all. An unpaired sample t - test was used to analyse significant differences of arterial pressure and systemic vascular resistance index (SVRI) related to the periods of measurement.

Results

Data of all 65 patients, 41 males and 24 females, were included into final analysis. Not a single patient suffered from any complication in the context of the present study. Age ranged between 39–81 years, with a mean age of 65 ± 3 years and a mean body mass index of 25.9 ± 2.8 kg/m2. Mean left ventricular ejection fraction was 0.62 ± 0.09. A total of 548 data pairs (T1: 288, T2: 260) were obtained during the study period. Unpaired t-test showed a significant difference (p < 0.05) between SVRI, heart rate and CI (CITPTD, CIPFX) before (T1) and after CPB (T2). Haemodynamic variables are shown in Table 1.
Table 1
Haemodynamic variables before and after cardiopulmonary bypass
 
pre - CPB
post - CPB
Variables
T1
T2
p
n = 288
n = 260
HR (min−1)
55 ± 5
81 ± 3
p < 0.05*
MAP (mmHg)
75 ± 4
74 ± 7
p = 0.68
SAP (mmHg)
114 ± 15
112 ± 13
p = 0.08
DAP (mmHg)
54 ± 11
53 ± 9
p = 0.43
CVP (mmHg)
9 ± 3
10 ± 2
p = 0.11
SVRITPTD (dynes∙s/cm5/m2)
1820 ± 73
1472 ± 109
p < 0.05*
CITPTD (L/min/m2) max
5.0 ± 0.5
5.3 ± 0.8
p < 0.05*
CITPTD (L/min/m2) mean
2.2 ± 0.5
2.9 ± 0.7
p < 0.05*
CITPTD (L/min/m2) min
1.2 ± 0.3
1.5 ± 0.6
p < 0.05*
CIPFX (L/min/m2) max
6.8 ± 0.6
7.0 ± 0.8
p < 0.05*
CIPFX (L/min/m2) mean
2.8 ± 0.6
3.4 ± 0.5
p < 0.05*
CIPFX (L/min/m2) min
1.1 ± 0.4
1.7 ± 0.7
p < 0.05*
CPB cardiopulmonary bypass, HR heart rate, MAP mean arterial pressure, SAP systolic arterial pressure, DAP diastolic arterial pressure, CVP central venous pressure, SVRI TPTD , systemic vascular resistance index measured by transpulmonary thermodilution CI TPTD , cardiac index by transpulmonary thermodilution, CI PFX cardiac index by autocalibrated semi-invasive pulse contour analysis
Values are given as maximum, mean and minimum ± SD
* p < 0.05 (vs. T1)
There was a moderate but significant correlation between CITPTD and CIPFX at T1 (r 2 = 0.34, p < 0.0001) and T2 (r 2 = 0.31, p < 0.0001) (Fig. 2). Bland-Altman analysis for CITPTD and CIPFX showed a mean bias of 0.65 L/min/m2, 95 % limits of agreement (LOAs) from −1.01 to +2.29 L/min/m2 before and a bias of 0.49 L/min/m2 with LOAs from −1.15 to +2.13 L/min/m2 after CPB. Percentage error (PE) was 63 % before and 50 % after CPB. Bias, LOAs and percentage errors for each time period (T1 - T2) are summarized in Table 2.
Table 2
Bland-Altman analysis showing bias, 95 % limits of agreement, confidence interval and percentage error before (T1) and after cardiopulmonary bypass (T2)
 
T1
T2
ndata/npatient
n = 288/n = 65
n = 260/n = 65
 
CIPFX
CIPFX
Mean (L/min/m2)
3.03
3.58
Bias (L/min/m2)
0.65
0.49
SD of bias (L/min/m2)
0.81
0.80
Confidence Interval of LOA (L/min/m2)
0.52
0.49
95 % limits of agreement (L/min/m2)
−1.01 to +2.29
−1.15 to +2.13
Percentage error (%)
63
50
CI PFX cardiac index by semi-invasive pulse contour analysis, CI of LOA confidence interval of the limits of agreement
Values are given as mean ± SD
There was a weak correlation between CIPFX and SVRI determined by transpulmonary thermodilution (SVRITPTD) and by pulse contour analysis (SVRIPFX) for both time periods (Fig. 3).
A PLR-manoeuvre before CPB was performed in all 65 patients. Responders increased their SVITPTD >15 % during PLR. We observed 37 responders (57 %) and there was a moderate correlation between CITPTD and CIPFX (r 2 = 0.28, p < 0.0001). During PLR, Bland Altman analysis showed a mean bias of 0.49 L/min/m2 and LOAs from −2.01 to +1.02 L/min/m2 with a percentage error of 68 % for CIPFX.
After exclusion of percentage changes <15 %, correlation coefficients between ∆CITPTD and ∆CIPFX were r 2 = 0.50, p < 0.0001 before and r 2 = 0.52, p < 0.0001 after CPB. Modified Bland-Altman analysis showed a bias of −4 %, with LOAs from −42 % to +33 % before CPB and of 0.18 % with LOA`s from −28 % to +29 % after CPB, respectively. Four quadrant plots revealed a concordance rate over 90 % indicating an acceptable ability for reflecting haemodynamic changes before and after CPB (Fig. 4a, b). Polar plot analysis demonstrated a poor trending ability before CPB (data within 10 % limits of agreement: 64 %, 20 % limits of agreement: 89 %) and an acceptable trending ability after CPB (data within 10 % limits of agreement: 71 %, 20 % limits of agreement: 93 %) for mean ∆CIPFX (Fig. 4c, d).
There was no significant correlation between femoral MAP and CIPFX before (r 2 = 0.01, p = 0.09) and after (r 2 = 0.001, p = 0.55) CPB.

Discussion

Our study demonstrated that semi-invasive autocalibrated arterial waveform analysis was not able to reliably measure CI compared with TPTD before and after CPB. The investigated monitoring system did not seem to be affected by SVRI and MAP. With respect to haemodynamic changes, the semi-invasive device showed an acceptable trending capability before and after CPB.
The recently introduced semi-invasive PulsioFlex monitoring system was developed to determine beat-to-beat CI and other variables such as SVI and SVRI by pulse contour analysis. A less invasive and easy to install method without the need for calibration could be advantageous in daily clinical practice, since it may decrease the reluctance of physicians to use advanced haemodynamic monitoring [12]. In the past, estimation of CI was mostly performed by pulmonary thermodilution, a time consuming technique which requires experience and is frequently associated with method related complications. In this context, quick availability, simple installation, easy interpretation of estimated values and less invasiveness are advantages for monitoring systems based on pulse contour analysis.
Today, clinicians can choose between a wide variety of less-invasive or non-invasive devices based on pulse contour analysis. Each device consists on a proprietary software algorithm and most of them are based on the findings by Otto Frank [13]. However, several studies demonstrated a lack of accuracy for these monitoring systems in the presence of changing vascular tone [14, 15]. A recent meta-analysis dealing with five different pulse contour monitoring systems revealed an acceptable accuracy in presence of haemodynamic stable conditions. However, the authors found higher percentage errors and bias in haemodynamic unstable patients compared with thermodilution [10]. There are only very limited data concerning the accuracy of the new PulsioFlex monitoring system. A recently published study investigated the PulsioFlex system in patients undergoing off-pump coronary artery surgery [16]. The authors found an acceptable accuracy for the semi-invasive device compared with transpulmonary thermodilution. Bland-Altman analysis revealed a slight underestimation of CI by pulse contour analysis with low bias and small LOA`s. Overall percentage error was slightly above the 30 % limit which was recommended by Critchley and colleagues [9]. Our findings were in contrast to these results. We found poor accuracy for the PulsioFlex monitoring system in haemodynamic stable patients and observed percentage errors which clearly indicate no interchangeability with the reference technique, transpulmonary thermodilution. A possible explanation for these conflicting results could be the underlying software algorithm. Based on the PiCCO algorithm (as used currently in the PiCCO2), the PulsioFlex monitoring system uses a modified version of Wesseling`s cZ algorithm. This algorithm analyses the actual shape of the pressure waveform with the focus on the dicrotic notch. After calculation of the exponential decay time by analysing the pressure curve following the dicrotic notch, pressure related compliance can be computed. The area under the systolic portion of the arterial pressure waveform is also taken into account [17, 18]. Keeping in mind that pressure curves differ from central to peripheral arteries [19, 20] the PiCCO system usually consists on a femoral artery catheter. The tip of the transpulmonary thermodilution catheter is located in the abdominal aorta leading to more central pressure waveforms. In this context, it must be noted that the above mentioned study which observed sufficient accuracy for the new semi-invasive device used the femoral artery signal as input for pulse contour analysis [16]. Interestingly, a recently published study investigated the PulsioFlex monitoring system in critically ill patients with a femoral arterial line and observed unreliability for estimation of absolute CI values but reliability for tracking CI changes [21]. This is of high clinical importance, as these systems may be often used as “add on” by using existing radial artery catheters. Recent studies could demonstrate that the location of the arterial catheter plays a major role concerning the accuracy of uncalibrated pulse contour analysis [22]. The PulsioFlex monitoring system is provided with an autocalibration mode, which calculates the initial CI by using patient specific data and an unique unpublished algorithm. Thereafter, estimation of CI is performed by the well known PiCCO2 pulse contour algorithm [17].
Keeping in mind, that there is a mathematical coupling between SVRI and CI, we observed a weak but significant correlation between SVRI and CI by pulse contour analysis. To evaluate the effect of SVRI on the differences of CI between techniques, we calculated the correlation between the bias of CIPFX and CITPTD and corresponding SVRI as suggested by recent literature [23]. We observed no significant correlation between the bias and SVRI before (r = −0.02, p = 0.79) and after (r = −0.07, p = 0.29) CPB. This result suggests that SVRI does not have a considerable impact on accuracy of CIPFX. In contrast, other studies, investigating an earlier PiCCO algorithm, showed an impairment of pulse contour analysis by changes in systemic vascular resistance [24]. However, we did not observe a significant relationship between CI by semi-invasive arterial waveform analysis and mean arterial pressure.
We studied this new monitoring system in patients undergoing elective coronary artery surgery under varying haemodynamic conditions, e.g. during a PLR manoeuvre before surgery. During the PLR manoeuvre, the semi-invasive monitoring system also failed interchangeability with the reference technique (CIPFX PE 68 %). As suggested by recent literature [25], we calculated the precision of CITPTD and CIPFX before and after CPB and found low coefficients of variation emphasizing our experience as we observed no rapid changes during data collection.
However, beside estimation of absolute values of CI, instantaneous tracking of haemodynamic trends could be extremely valuable for the clinician in the decision making process related to haemodynamic optimization. As recommended by recent literature, we excluded changes of CI obtained by transpulmonary thermodilution <15 % from further analysis [26]. Based on these criteria, concordance rates over 95 % indicate good trending ability, rates between 90–95 % are acceptable and concordance rates below 90 % should be considered as poor trending. The semi-invasive system overestimated absolute values of CI but showed an acceptable ability for following trends before and after CPB. It must be noted, however, that if exclusion zones were not applied, concordance rates in our study fell below 90 %. This could be explained by a central zone effect, respectively by the exclusion zone. Data points close to the center of the four quadrant plots represent small CI changes. These changes are most probably due to random error effects and therefore do not represent true CI changes. In addition, with respect to distribution of measurement errors, a precision of 20 % is considered as the upper limit of acceptance when using a reference method such as thermodilution. Therefore, exclusion of data points by an exclusion zone of 0.5–1.0 L/min or 15 % is considered as the gold standard. Interestingly, exclusion zones can be reduced to 5 and 10 % when an aortic flowprobe is applied as the reference technique [26]. With respect to trending ability, our findings were in agreement with other studies dealing with uncalibrated pulse contour analysis [27]. However, recent literature emphasized statistical limitations of four quadrant plots and recommended polar plots for trending analysis [28]. In our study, polar plot analysis revealed a poor trending ability before CPB and an acceptable trending of changes in CI after CPB for the investigated autocalibrated monitoring system. With respect to trending ability, a recent published investigation demonstrated poor trending for the new semi-invasive monitoring system in patients undergoing off-pump cardiac surgery [16]. Due to a small number of patients and possible random observation, the authors emphasized careful interpretation of their trending results. However, a recent study dealing with perioperative haemodynamic optimization by autocalibrated pulse contour analysis for CI trending was able to show a reduction in postoperative complications [29].
Some limitations must be emphasized in our study.
We excluded patients with haemodynamic instability, shock or lack of sinus rhythm and investigated patients undergoing elective coronary surgery with normal left ventricular function and without continuous high-dose (>0.1 μg/kg/min) catecholamine therapy. Therefore, our results cannot be extrapolated to patients with impaired left ventricular function, low cardiac output, cardiac arrhythmias or patients receiving continuous high-dose inotropic or vasoactive support.
Due to interferences of thermodilution curves caused by temperature fluctuations, transpulmonary thermodilution as the reference technique has some limitations especially after CPB. The probable reason for these transient thermal changes might be an influx of cold blood from hypoperfused compartments during CPB [30, 31]. In addition, accuracy of pulse contour analysis may also be affected by CPB. Recent investigations demonstrated abnormal aortic-to-radial arterial pressure gradients following CPB [32]. Future studies should investigate the reliability of this semi-invasive monitoring system in critically ill patients with both a femoral and a radial artery signal as input for pulse contour analysis.

Conclusions

In conclusion, we observed poor accuracy for the new pulse contour monitoring system before and after CPB compared with transpulmonary thermodilution in patients undergoing coronary artery surgery. Furthermore, the semi-invasive device failed to meet criteria of interchangeability during a PLR-manoeuvre. There was a no significant influence of SVRI and MAP on CI by semi-invasive pulse contour analysis. However, we obtained an acceptable reliability for tracking changes of CI by the new semi-invasive monitoring system after CPB. Since we investigated only a homogeneous elective patient population, the present results cannot be readily transferred to other groups of patients.

Acknowledgements

The authors are indebted to Bernd Kuhr for excellent technical assistance and logistic support.
Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://​creativecommons.​org/​licenses/​by/​4.​0/​), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://​creativecommons.​org/​publicdomain/​zero/​1.​0/​) applies to the data made available in this article, unless otherwise stated.

Competing interests

Dr. Bein is a member of the medical advisory board of Pulsion Medical Systems (Munich, Germany) and has received honoraria for consulting and giving lectures.
Dr. Renner has received honoraria from Edwards Lifesciences (Irvine, CA, USA) for giving lectures.
Dr. Gruenewald has received honoraria from GE Healthcare (Munich, Germany) for giving lectures. All other authors declare no competing interests.

Authors’ contributions

OB conducted the study, analyzed the data and drafted the manuscript. JC and CF conducted the study. MM and AC has made substantial contributions to data acquisition and has been involved in drafting the manuscript. MA and MG participated in statistical analysis and helped to draft the manuscript. JH has made contributions to data analysis and study design. MSo participated in data analysis and coordination of the study. MSt has been involved in drafting the manuscript and participated in study design. JR participated in study design and coordination and helped to draft the manuscript. BB conceived of the study, helped with drafting the manuscript and data analysis. All authors read and approved the final manuscript.

Authors` information

OB works as a consultant at the Department for Anaesthesiology and Intensive Care Medicine, University Hospital Schleswig-Holstein, Campus Kiel. His clinical focus area is anaesthesia in cardiac surgery and paediatric cardiac surgery. Research interests are haemodynamic monitoring, fluid therapy and patient outcome.
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Metadaten
Titel
Accuracy of an autocalibrated pulse contour analysis in cardiac surgery patients: a bi-center clinical trial
verfasst von
Ole Broch
Jose Carbonell
Carlos Ferrando
Malte Metzner
Arne Carstens
Martin Albrecht
Matthias Gruenewald
Jan Höcker
Marina Soro
Markus Steinfath
Jochen Renner
Berthold Bein
Publikationsdatum
01.12.2015
Verlag
BioMed Central
Erschienen in
BMC Anesthesiology / Ausgabe 1/2015
Elektronische ISSN: 1471-2253
DOI
https://doi.org/10.1186/s12871-015-0153-2

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