Introduction
Ventilator-associated pneumonia (VAP) is the most common acquired infection in critically ill patients under mechanical ventilation [
1], often associated with significant morbidity [
2,
3]. VAP is mainly precipitated by microaspiration of contaminated gastric and oropharyngeal secretions [
4]. Microaspiration is defined by leakage of oropharyngeal secretions accumulated upstream the tracheal cuff into the lower respiratory tract [
5,
6]. The gold standard test for the diagnosis of microaspiration is using technetium 99 m [
7]. However, applying this technique in intubated patients in the intensive care unit (ICU) is thwarted by the difficulty of transporting patients to the radiology department to avoid radioactivity in ICU [
8]. Pepsin comes from pepsinogen and is secreted by the chief cells in the stomach, and amylase is a digestive enzyme, secreted by the salivary glands and the pancreas. Because they are not normally present in the respiratory tract, pepsin, and salivary amylase were proposed to diagnose microaspiration of gastric content and oropharyngeal secretions, respectively [
9‐
12]. Their use in intubated critically ill patients is rapid, easy to perform in routine, cheap and only requires tracheal secretions.
Over the past decade, transesophageal echocardiography (TEE) has emerged as a common, minimally invasive, bedside examination in ICU [
13], with a low complication rate in intubated patients [
14,
15]. TEE-induced bacteremia is extremely rare; thus, TEE is not an indication for antibiotic prophylaxis [
16]. Nevertheless, potential microaspiration associated with TEE has never been evaluated in intubated ICU patients. TEE could indirectly trigger microaspiration of oropharyngeal and gastric contents in mechanically ventilated patients via factors such as loss of integrity of the esophageal sphincter, gastroesophageal reflux, displacement of tracheal tube, and modification of tracheal cuff inflation.
The main objective of this study was to evaluate the role of TEE in triggering microaspiration of gastric contents and oropharyngeal secretions, and VAP in intubated critically ill patients.
Methods
Study design and participants
We performed a multicentric prospective observational study in four French medical ICUs of university hospitals between March 2017 and September 2018. Consecutive adult patients intubated and mechanically ventilated for more than 24 h prior to enrollment and who required TEE were included. Exclusion criteria were pregnancy, tracheostomy, and TEE contraindications. This study was conducted in compliance with the amended Declaration of Helsinki. The protocol was approved by the ethical committee CPP, Ile de-France III (EUDRACT number: 2016-A01488-43, approval number: S.C.3457). The protocol was considered as a component of standard care, and patient consent was waived. Written and oral information about the study was given to patients or families.
Procedures and definitions
All included patients were subjected to endotracheal suction just before TEE and within the two hours after. For quantitative analyses, endotracheal aspirates were drawn without the addition of saline beforehand. The collected endotracheal aspirates were stored at − 20 °C in each center and sent to a central laboratory (Lille University Hospital) at the end of the study. All measurements of pepsin and amylase were performed by biologists who were blinded to the chronological status of TEE samples (before vs. after TEE). Pepsin was quantitatively measured by ELISA technique, and salivary amylase activity was calculated as the difference between total and pancreatic amylase activities [
12,
17]. The tracheal cuff pressure was manually checked before and after TEE. For some patients included in the Henri Mondor center, Creteil, the tracheal cuff pressure was continuously and mechanically assessed from five minutes before TEE until five minutes after. For those patients, the tracheal cuff pressure signal was recorded using differential pressure transducer TSD160D (Biopac Systems, Goleta, CA, USA) connected to analog/numeric data acquisition system (MP150, Biopac systems, Goleta, CA, USA) and stored on a computer to be analyzed with AcqKnowledge software version 5.0 (Biopac systems, Goleta, CA, USA).
Microaspiration of gastric contents and oropharyngeal secretions is usually confirmed upon detecting significant pepsin (> 200 μg/L) [
17] and salivary amylase (> 1685 IU/L) [
12] concentrations in the tracheal secretions, respectively. TEE-associated microaspiration of gastric contents (or oropharyngeal secretions) was defined by the association of: (1) pepsin (or salivary amylase) concentration which is ≥ 50% higher in the post-TEE sample than in the pre-TEE sample and (2) a significant post-TEE concentration of pepsin of > 200 μg/L (or salivary amylase of > 1685 IU/L).
VAP diagnosis relied on clinical, radiological, and microbiological criteria. Namely, new and persistent infiltrate on chest X-rays (CXR) was associated with two of the following criteria: (1) turbid tracheal aspirates; (2) temperature > 38 °C or < 36 °C; and (3) peripheral leukocyte count > 10 G/L or < 1.5 G/L). All VAP diagnoses were documented by a positive microbiological sample of tracheal aspirate (≥ 10
5 CFU/mL), protected telescopic catheter liquid (≥ 10
3 CFU/mL), or bronchoalveolar lavage (≥ 10
4 CFU/mL). Tracheobronchial colonization was confirmed by a positive (≥ 10
5 CFU/ml) tracheal aspirate without CXR signs of VAP [
18]. The participating ICUs management fulfilled the VAP-prevention guidelines [
18,
19].
Data collection
All data were prospectively collected starting with the inclusion data: age, gender, body mass index, simplified acute physiology score II (SAPS II) at ICU admission [
20], comorbidities, history of acute respiratory distress syndrome, shock, and VAP prior to TEE, date and cause of intubation, tracheal tube characteristics (type, diameter, position), Sequential Organ Failure Assessment (SOFA) score, Richmond Agitation and Sedation Scale (RASS), duration of mechanical ventilation prior to TEE, time between last oral decontamination and TEE, ventilator parameters, tracheal cuff pressure before and after TEE, gastric tube and enteral feeding management, evaluation of residual gastric volume, concomitant treatments, probe type and introduction (duration, number of attempts, method, patient position), TEE characteristics (date, duration, indication, use of transgastric view), and complications. The following data were collected during ICU stay: length of stay, mechanical ventilation duration, VAP, and mortality.
Outcomes
The primary endpoint of this study was the percentage of patients with TEE-associated microaspiration of gastric contents and/or oropharyngeal secretions. The secondary outcomes were the percentage of patients who developed VAP within three days after TEE and the evolution of tracheal cuff pressure throughout TEE procedure.
Statistical analysis
Statistical analysis was performed using JMP software (version 9; SAS Institute Inc, Cary, NC) and GraphPad Prism 5 software (GraphPad Software Inc., La Jolla, CA, USA). The number of patients required to assess the incidence rate of microaspiration during TEE was estimated at 75, considering a theoretical prevalence of 75% (previous studies reported the presence of microaspiration at baseline in at least 50% of intubated patients) [
12,
21,
22], a precision of ± 10%, a confidence interval of 95%, and a type I error rate of 5%. We anticipated a 25% failure rate for sample processing and analysis and decided to include a total of 100 patients.
Normality of variables was evaluated by Shapiro–Wilk test. Continuous variables were expressed as mean (± standard deviation) or median (first quartile–third quartile) according to their Gaussian or non-Gaussian distribution, respectively. We compared patients who developed VAP within the three days following TEE with their counterparts using Student t test for Gaussian continuous variables, Mann–Whitney test for non-Gaussian continuous variables, and Chi-square or Fisher exact tests for categorical variables, as appropriate. We compared concentrations of pepsin and salivary amylase before and after TEE using paired Wilcoxon test. We evaluated the change in tracheal cuff pressure throughout TEE procedure using one-way ANOVA and Dunnett multiple comparison test. For all tests, a two-tailed P < 0.05 was considered statistically significant.
Discussion
To the best of our knowledge, this is the first study conducted to evaluate the impact of performing TEE on the occurrence of microaspiration and VAP in intubated critically ill patients. Although a substantial number of patients could be characterized as having TEE-associated microaspirations (23%), according to an ad hoc definition, the changes in pepsin and salivary amylase levels throughout TEE process showed huge interindividual variability. We detected no association between TEE-associated microaspiration and the development of VAP during the three days following TEE. However, because of the high rate of VAP observed after TEE and the limitations of our methods, our findings cannot formally rule out a role for TEE in the occurrence of VAP. TEE generated a transient variation of tracheal cuff pressure, especially upon inserting and removing the TEE probe.
Microaspiration is a well-known causative factor of VAP [
23]. Pepsin and salivary amylase are reliable markers of microaspiration and are tightly linked to the development of VAP [
21,
24,
25]. These markers have been used as surrogates in studies evaluating the efficacy of various devices in preventing VAP, as tracheal tubes [
26], subglottic secretion drainage systems [
27], and mechanical devices controlling tracheal cuff pressure [
17]. In such studies, microaspiration assessment relied on several tracheal aspirates drawn over a wide timeframe (1 or 2 days), and its definition considered the percentage of tracheal aspirates with higher levels of pepsin (> 200 μg/L) and/or salivary amylase (> 1685 IU/L). For us, it was not possible to evaluate TEE-associated microaspiration using the same approach given the limited number of tracheal aspirates available in our protocol (only two/patient). Of more, we relied on commonly reported thresholds for salivary amylase and pepsin [
8,
12,
26].
The continuous monitoring of tracheal cuff pressure throughout TEE procedure showed significant elevation of cuff pressure, especially during insertion and removal of the TEE probe. Persistent underinflation (< 20 cmH
2O) of the tracheal cuff was shown as an independent risk factor for microaspiration and VAP [
28], whereas cuff leakage was inversely correlated with cuff pressure [
29]. Hypothesizing that acute variations of tracheal cuff pressure during TEE might be associated with microaspiration and VAP warrants further research.
The relatively high rate of VAP found in this study can be reasonably attributed to the severe cases we included. Of note, 38% of patients presented with acute respiratory distress syndrome. However, we cannot formally exclude a role of microaspiration in this high rate. The fact that patients who caught VAP had their tracheal tubes larger than those used in patients who did not may suggest more leaks occurring in the former group. Moreover, patients who caught VAP were more often on anticoagulant, a therapy that has potential anti-inflammatory effects beyond anticoagulation, and which may be beneficial in acute respiratory distress syndrome [
30]. For instance, nebulized heparin was proposed for lung injury but with contradictory results [
31] and was not effective in preventing VAP [
32].
We did not identify any dreaded clinical complication associated with TEE neither did TEE significantly impact salivary amylase and pepsin concentrations. However, the substantial levels of pepsin and amylase observed in some patients and the fact that VAP patients had endured more attempts of TEE probe introduction might represent a good incentive to install some VAP prevention measures before and/or during TEE. Such measures may involve deep oropharyngeal suctioning [
33], subglottic suctioning [
34], semi-recumbent positioning [
35], continuous control of tracheal cuff pressure [
17], or using higher PEEP levels [
29].
This multicenter study was conducted in four tertiary university ICUs where TEE is routinely used in intubated critically ill patients. The major strengths of the study are the comprehensive search for risk factors for microaspiration, its prospective design, the combined use of salivary amylase and pepsin for microaspiration documentation, and the continuous assessment of tracheal cuff pressure to scrutinize VAP pathophysiology. Our study has several limitations. First, the cohort included a relatively small number of patients with no control arm. Second, pepsin and salivary amylase and tracheal cuff pressure continuous monitoring were not assessed in all patients. Third, the definition of TEE-associated microaspiration may be questionable, as previously discussed. It used a single assessment of biomarkers and an arbitrary cutoff. We did not correct for baseline concentration of biomarkers in the digestive tract, but these biomarkers are not normally found in the respiratory tract and previous studies did not use such corrections. Fourth, the use of three days as a cutoff point to define VAP after TEE is also questionable, but results were similar upon using a five-day cutoff point. Fifth, we focused on direct microaspiration during TEE and did not assess other mechanisms that may cause pneumonia, as dysphagia or swallowing dysfunction [
36]. Eventually, we did not assess the change in tracheal bacterial colonization. The amount of bacterial inoculum could be used as a closer surrogate for VAP [
37]. Sixth, VAP would have been more relevant as a primary endpoint from a clinical point of view. However, if TEE has a potential impact on VAP, it is likely to be small given the multiple factors influencing VAP occurrence. We therefore used microaspiration as the primary endpoint because microaspiration is considered as the main mechanism of VAP. Lastly, the limitations of the methods used to identify TEE-associated microaspiration and the high rate of VAP observed after TEE cannot allow ruling out a role for TEE.
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