Background
SARS-CoV-2 infection can be complicated by the development of an acute respiratory distress syndrome (COVID-19 ARDS) associated with high mortality rate. The severity of the lung injury often requires mechanical ventilation [
1‐
3], and recently, some morphological pathways of the COVID-19-related ARDS have been elucidated in a series of autopsies. The histologic analysis of pulmonary vessels showed widespread thrombosis with microangiopathy [
4], diffuse alveolar damage, capillary congestion, necrosis of pneumocytes, interstitial and intra-alveolar edema and platelet–fibrin thrombi [
5]. These results suggest that the profound hypoxemia that these patients might experience can be due to both epithelial and endothelial injury. Nonetheless, an in vivo description of the evolution of the disease is still lacking. Biomarkers evaluation can help to understand COVID-19 pathogenesis over-time. This approach may have clinical implications, helping to clarify the characteristics of this peculiar ARDS and, further, enhancing the chances of treatments of this disease.
Angiopoietin-2 (Ang-2), soluble intercellular adhesion molecule-1 (ICAM-1), soluble vascular cell adhesion molecule-1 (VCAM-1), P-selectin, E-selectin are used as biomarkers of endothelium injury, whereas receptor for advanced glycation end-products (RAGE) is considered a marker for alveolar epithelial injury [
6]. Previous studies showed the usefulness of these biomarkers in predicting worse outcomes in patients with “classical” ARDS, including mortality [
7‐
9]. Unfortunately, besides studies focused on markers of systemic endothelial dysfunction, such as D-dimers [
10], few data are available on other biomarkers in COVID-19-related ARDS. This is relevant since it is not yet established whether the evaluation of biomarkers used in classical ARDS patients could have a prognostic relevance even in COVID-19 ARDS.
Some authors advocate that significant differences exist between classical and COVID-19-related ARDS, the latter being characterized by higher respiratory system compliance [
11,
12] and lower recruitability [
13,
14]. On the other hand, other authors do not recognize differences between the two types of ARDS since a large observational study suggests similar pathophysiological features and outcomes [
15].
The aim of this study was to evaluate whether the plasma levels of “endothelial” and “alveolar” biomarkers (Ang-2, ICAM-1, VCAM-1, P selectin, E-selectin and RAGE) vary over time between survivors and non-survivors in COVID-19-related ARDS patients. Furthermore, we compared the biomarkers expression in COVID-19-related and classical ARDS.
Methods
Study design
The present analysis is based on data from the Pro-thrombotic Status in Patients With SARS-Cov-2 Infection (ATTAC-Co) study (ClinicalTrials.gov Identifier: NCT04343053). The ATTAC-co was a prospective, single-centre study performed at the University Hospital of Ferrara (Italy). The present analysis is specifically designed to investigate the relationship between several biomarkers that are indicators of epithelial and endothelial lung injury in consecutive patients with confirmed COVID-19 who were admitted to COVID-19-dedicated Intensive Care Unit between April and June 2020 and needed mechanical ventilation. A group of patients, admitted in the same period in the non-COVID-dedicated ICU, with similar clinical characteristics in terms of ARDS presentation, but negative for SARS-CoV-2 infection were also included as controls. Mechanical ventilation settings in both groups included constant-flow controlled ventilation, a tidal volume of 6 ml/kg of ideal body weight and the PEEP level titrated to the lowest driving pressure. All patients gave their written informed consent. In case of unconsciousness, the informed consent was signed by their next of kin or legal authorized representative.
Study population
Inclusion criteria were: (a) age > 18 years; (b) confirmed SARS-CoV-2 infection; (c) need of invasive mechanical ventilation; (d) meeting the Berlin criteria definition for ARDS. Patients were excluded from the study in case of pregnancy or do-not-resuscitate order. SARS-CoV-2 infection was confirmed by reverse transcriptase-polymerase chain reaction assay (Liaison MDX, Diasorin, Saluggia, Italy) from nasopharyngeal swab specimen or tracheal aspirate. Clinical management was in accordance with current guidelines and specific recommendations for the COVID-19 pandemic by Health Authorities and Scientific Societies [
16].
Procedures and blood samples
At ICU admission, clinical and physiological variables were collected: age, sex, body mass index (BMI), Sequential Organ Failure Assessment (SOFA) Score, Simplified Acute Physiology Score (SAPS) II, comorbidities and main laboratory data. Respiratory data collected were: ratio of partial pressure of arterial oxygen to fractional concentration of inspired oxygen (PaO2/FiO2), partial pressure of carbon dioxide (PaCO2), end-inspiratory plateau pressure (assessed performing a 5-s end-inspiratory occlusion), positive end-expiratory pressure (PEEP), tidal volume for predicted body weight (Vt/PBW) and static compliance of the respiratory system calculated as tidal volume/(end inspiratory plateau pressure–total PEEP).
Three different samples of venous blood were collected: at the inclusion in the study (T1, after 1 [
1,
2] days from start of MV), after 7 ± 2 days (T2) and 14 ± 2 days (T3). Blood withdrawn was performed from an antecubital vein using a 21-gauge needle. All patients underwent blood sampling in the early morning. The first 2 to 4 mL of blood was discarded. The serum and plasma samples were stored at -80 °C. The plasma levels of Ang-2, ICAM-1, VCAM-1, P-selectin, E-selectin and RAGE, were determined with a bead-based multiplex immunoassay (Luminex, Thermo Fisher Scientific, Waltham, MA, USA). The latter laboratory analyses were performed in the Translational Research Center of the Maria Cecilia Hospital, Cotignola (RA), Italy.
Simultaneously to each blood sample, gas exchanges and respiratory mechanics variables were collected.
Outcomes
The primary outcome was to evaluate the trend of the biomarker’s plasma levels in survivors and non-survivors COVID-19 ARDS patients. The secondary outcome was the differences in respiratory mechanics variables and gas exchanges between survivors and non-survivors. Furthermore, we compared the biomarkers’ plasma levels at T1 in patients with COVID-19-related ARDS and classical ARDS. Finally, we compared clinical characteristics and plasma levels of the biomarkers at ICU admission between patients with COVID-19-related ARDS and classical ARDS. The dataset of classical ARDS was prospectively registered during the same study period, enrolling all consecutive ARDS patients admitted to a non-COVID-19-dedicated ICU at Ferrara Hospital.
Statistical analysis
Continuous variables with normal distribution were expressed as mean ± SD. Continuous variables with a non-normal distribution were expressed as median and interquartile range. Normal distribution of the variables was tested with the Kolmogorov–Smirnov test. The variables normally distributed were compared by t test; otherwise the Mann–Whitney U was used. Categorical variables were summarized in terms of numbers and percentages and compared using the two-sided Fisher’s exact test. Differences between measurements were analyzed using repeated-measures ANOVA or two-sample Kolmogorov–Smirnov analysis for data with normal or not normal distribution, respectively. When multiple comparisons were made, p values were adjusted by the Bonferroni post hoc procedure. Receiver operator characteristic (ROC) curves were used to analyze the biomarkers’ ability of to predict 90-day mortality. ROC curve analyses are reported as AUROC, with a 95% confidence interval (95% CI). Due to the unpredictable nature of the COVID-19 outbreak, we were unable to assume an “a priori” sample size; as a convenience sample size, we enrolled all consecutive patients with confirmed COVID-19 who were admitted to two COVID-19-dedicated Intensive Care Unit between April and June 2020.
For all comparisons, a p value of ≤ 0.05 was considered statistically significant. When appropriate, 95% confidence intervals (CIs) were calculated. All analyses were performed with SPSS 25 (IBM, USA).
Discussion
Our study highlights that a substantial differences exist in COVID-19-related and classical ARDS, as the biomarkers levels of endothelial injury, such as Ang-2 and ICAM-1, were higher in COVID-19-related ARDS, supporting a different pathophysiological pathway of these two syndromes, as recently suggested [
11,
17]. Furthermore, we found that some biomarkers of pulmonary endothelial injury, Ang-2 and ICAM-1, are significantly higher in non-survivors patients with COVID-19-related ARDS than in survivors. Conversely, the levels of a biomarker of alveolar epithelial injury, the RAGE, were not different. Our findings suggest that the endothelial injury pathway may be predominant in the pathogenesis of more severe forms of COVID-19-related ARDS.
Previous studies have shown that higher levels of Ang-2 are related to an increased pulmonary vascular leak [
18,
19] and that the pulmonary vascular endothelium to up-regulate the ICAM-1 expression in response to inflammation [
8,
12]. Other authors found that ICAM-1 can bind alveolar macrophages and enhance inflammatory cytokine production in the alveoli [
20]. We found that the plasma levels of Ang-2 and ICAM-1 at T1 were higher in non-survivors than in survivors and, furthermore, i.e., that the plasma levels of Ang-2 and ICAM-1 increased rapidly in COVID-19 non-survivors, within 24 h from ICU admission. To this end, our data might suggest that in COVID-19 ARDS patients the extent of pulmonary endothelium injury, as reflected by ICAM-1 levels, sustains the overall pulmonary inflammation and contribute to the pathogenesis of alveolar epithelial injury. Of note, we found a correlation between ICAM-1 level at admission and worsening of respiratory system compliance during the ICU stay. We thus speculate that evolution of COVID-19-related ARDS toward a more severe phenotype could be related to the extent of pulmonary endothelium injury in the early phase of the disease. Remarkably, the D-dimer levels, a widely used prognostic marker in COVID-19 patients [
10,
21,
22]), did not differ between survivors and non-survivors within 24 h from ICU admission.
We were unable to detect any differences in RAGE levels between survivors and non-survivors at ICU admission and throughout the ICU stay. Moreover, the RAGE levels were lower than those previously described in the context of classical ARDS [
9]. Since higher RAGE levels have been previously associated with clinical outcomes in patients with classical ARDS, several considerations should be made:
firstly, alveolar epithelial damage is a less reliably measure when compared to endothelial injury; in this connection, reduced RAGE expression has been reported in patients with idiopathic pulmonary fibrosis, where alveolar epithelial injury is common, and a high prevalence of lung fibrosis is suspected in COVID-19-related ARDS survivors [
23];
secondly, it has been hypothesized that decreased circulating RAGE could be a marker of deficient inflammatory control [
24].
Finally, low plasma RAGE was described in respiratory failure due to COPD [
25]. It should be noted that RAGE levels may reflect differing mechanisms of lung injury in different lung diseases [
24] and hence we can only speculate that the pulmonary endothelial injury is predominant in COVID-19 ARDS, when compared to alveolar injury.
Interestingly, Gattinoni et al. hypothesized that two different COVID-19 ARDS phenotypes can be detected: the first characterized by high compliance and lower recruitability, the second characterized by low compliance and higher recruitability [
11]. In a post hoc analysis, we found higher values of Ang-2 and E-selectin in patients with higher compliance. Nonetheless, due to the low number of COVID patients with low compliance, larger cohort studies are warranted to scrutinize the biomarkers associated with different phenotype(s) of COVID-19–related ARDS.
When comparing COVID-19-related ARDS with a cohort of patients with classical ARDS, we observed a significant difference in all the evaluated biomarkers. Ang-2 and ICAM-1 were higher in COVID-19-related ARDS, further highlighting the role of pulmonary vascular injury in this context. On the other hand, RAGE was higher in classical ARDS patients. P-selectin was higher in classical ARDS patients, whereas E-selectin was higher in COVID-19-related ARDS (Table
3). The different behavior of these two-selectin markers further highlights the predominant role of the endothelium, the primary source of E-selectin [
26], in the genesis of COVID-19-related ARDS.
This is a hypothesis-generating study, and we must acknowledge some limitations. First, this is a single-centre prospective study focused on the description of pathological alteration in COVID-19-related ARDS. The clinical relevance of these findings should be confirmed in future interventional studies. Secondly, we enrolled patients needing mechanical ventilation and thus our results could not be extended to mild or moderate COVID-19. Third, recent findings suggest that combining respiratory system compliance with D-dimer values can better characterize patients with COVID-19 ARDS; nonetheless, we were unable to perform this analysis due to the fact that almost all our patients (28/31) had D-dimer levels higher than 1880 ng/mL, the cutoff suggested to distinguish between low and high D-dimer [
10]. Furthermore, our study investigated multiple biomarkers of endothelial dysfunction and only one marker of epithelial injury. The choice of RAGE as only marker of alveolar epithelial injury, even if consistent with recent studies [
27‐
30], must take into account the intrinsic limits of that biomarker (for example, its ubiquity distribution); additional biomarkers of endothelial injury, such as surfactant protein-D, would have strength our findings.
Publisher's Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.