Introduction
Microvascular capillary leakage resulting in tissue edema, vasodilation refractory to vasopressors, and increased recruitment of leukocytes denote key features of sepsis-related endothelial-cell activation. During the course of severe sepsis and septic shock, widespread endothelial cell activation contributes to the initiation and progression of multi-organ failure
Ang-1 and Ang-2 are antagonistic ligands, which bind to the extracellular domain of the Tie2 receptor, which is almost exclusively expressed by endothelial cells
Beyond its role as a mediator, Ang-2 has been identified as a promising strong marker of endothelial activation in various diseases
To address these issues, we wanted to study the time course of Ang-2 release, and the association of Ang-2 with soluble adhesion molecules and inflammatory cytokines in a graded and well-defined human endotoxemia model. Therefore, we re-measured circulating Ang-2, cytokines, and adhesion molecules in blood samples from a placebo-controlled interventional trial on pharmacologic p38 mitogen-activated protein (MAP) kinase inhibition during experimental human endotoxemia
Materials and methods
Subjects
Twenty-one healthy male subjects, mean age 29 (range 19 to 44) years, were admitted to the research unit of our ICU (Medical Department) at University Medical Center of Groningen, Groningen, The Netherlands. The local Medical Ethics Committee approved the study and written informed consent was obtained from the subjects. A radial arterial catheter was placed for blood sampling. Thirty minutes before the infusion of lipopolysaccharide (LPS), the volunteers received a single oral dose of RWJ-67657 (4-(4-(Fluorophenyl)-1-(3-phenylpropyl)-5-(4-pyrindinyl)-1H-imidazol-2-yl)-3-butyn-1-ol), supplied in an oral pharmaceutical formulation (R.W. Johnson Pharmaceutical Research Institute, Bassersdorf, Switzerland). Three dose levels were tested, placebo-controlled: placebo (n = 6), 350 mg (n = 5), 700 mg (n = 6), and 1400 mg (n = 4). At time point t = 0, LPS (
Patients
The time course of Ang-2 release during the early course of human sepsis was studied in 21 ICU patients (Internal Medicine Department) recruited at Hannover Medical School (tertiary care university hospital), Hannover, Germany. Patient characteristics are shown in Table
Characteristics of septic ICU patients on admission
Characteristics
Value
Patients, number
21
Male
8 (38.1%)
Female
13 (61.9%)
Age, years, median (min to max)
57 (36 to 72)
Reason for medical ICU admission
Pneumonia
12 (57.1%)
Peritonitis
4 (19.0%)
Urinary tract infection
2 (9.5%)
Systemic mycosis
2 (9.5%)
Endocarditis
1 (4.8%)
Mediastinitis
1 (4.8%)
Mean arterial pressure (mmHg)
78 (58 to 108)
Heart rate (beats/minute)
95 (53 to 125)
Vasopressor support, number
12 (57.1%)
Mechanically ventilated, number
19 (90.5%)
Fraction of inspired oxygen (%)
40 (25 to 95)
APACHE II score
22 (12 to 48)
SOFA score
10 (3 to 19)
Mortality, number
11 (52.4%)
APACHE = Acute Physiology and Chronic Health Evaluation; ICU = intensive care unit; SOFA = Sequential Organ Failure Assessment.
Quantification of circulating angiopoietin-1 and 2, and soluble Tie2
Ang-1 and Ang-2 were measured by in-house immuno luminometric assay (ILMA), and ELISA as previously described
Quantification of soluble endothelial-adhesion molecules and cytokines
Soluble ICAM-1, E-selectin, and P-selectin were measured using Fluorokine® MultiAnalyte Profiling kits and a Luminex® Bioanalyzer (R&D Systems, Oxford, UK) according to the manufacturers' instructions. TNF-alpha, IL-6, IL-8, and c-reactive protein (CRP) were determined using Medigenix Easia kits from BioSource (BioSource, Nivelles, Belgium) and reported previously
Statistical analysis
The modified Kolmogorov-Smirnov test was used to test for a normal distribution of continuous variables. In the human endotoxemia model, a non-parametric analysis of variance (ANOVA) (Friedman's test) with Dunn's test for multiple comparison (two-sided) was used to demonstrate statistical changes in Ang-2, cytokines, and adhesion molecules. Correlations of Ang-2 with TNF-alpha, E-selectin, and the heart rate/mean arterial pressure index were calculated with Pearsons's correlation and linear regression analysis after log-transformation. Data are presented as mean ± standard error of the mean unless otherwise stated.
In patients, differences between survivors and non-survivors at baseline and during follow-up were compared by non-parametric two-sided Mann Whitney U test. Receiver operator characteristic (ROC) procedures identified optimal cut-off values for Ang-2 to differentiate between survivors and non-survivors. Contingency table-derived data and likelihood ratios were calculated using the StatPages website
Results
Angiopoietin-2 is released in a distinctive pattern after endotoxin challenge in healthy volunteers
Normal Ang-2 concentrations (0.57 ± 0.20 ng/mL) were present at baseline in healthy volunteers (Table
Time course of Ang-2, cytokines, and adhesion molecules after LPS challenge in healthy subjects
Time course of Ang-2, cytokines, and adhesion molecules after LPS challenge in healthy subjects. (a) Concentrations of circulating angiopoietin (Ang)-2 compared with plasma levels of TNF-alpha. IL-6, IL-8, and C-reactive protein (CRP) after lipopolysaccharide (LPS) challenge in six healthy volunteers. (b) Concentrations of circulating Ang-2 compared with plasma levels of endothelial adhesion molecules E-selectin, P-selectin, and inter-cellular adhesion molecule-1 (ICAM-1) after LPS challenge in six healthy volunteers. Non-parametric analysis of variance (Friedman's test) with Dunn's test for multiple comparison (two-sided) was used to demonstrate statistical changes in Ang-2, cytokines, and adhesion molecules (y-axes denote percentage increase; baseline = 100%).
Time course after LPS challenge in healthy subjects
Time course after LPS challenge
Variables
Pre-dose
1 hour
1.5 hours
2 hours
2.5 hours
3.5 hours
4.5 hours
6.5 hours
8 hours
24 hours
Systolic BP (mmHg)
140 ± 14
139 ± 11
152 ± 11
158 ± 18
151 ± 18
142 ± 22
121 ± 18
107 ± 11
104 ± 11
131 ± 11
< 0.0001
Diastolic BP (mmHg)
74 ± 10
74 ± 7
80 ± 7
77 ± 12
65 ± 12
61 ± 14
54 ± 11
55 ± 8
55 ± 7
66 ± 7
< 0.0001
MAP (mmHg)
96 ± 11
96 ± 9
104 ± 7
104 ± 13
94 ± 14
88 ± 16
77 ± 13
72 ± 8
71 ± 7
88 ± 7
< 0.0001
Heart rate (beats/minute)
61 ± 16
59 ± 11
78 ± 19
78 ± 18
92 ± 12
98 ± 8
101 ± 8
97 ± 11
96 ± 13
81 ± 16
< 0.0001
HR/MAP index
0.64 ± 0.11
0.62 ± 0.11
0.75 ± 0.17
0.76 ± 0.22
1.01 ± 0.22
1.15 ± 0.26
1.36 ± 0.32
1.36 ± 0.27
1.4 ± 0.22
0.92 ± 0.16
< 0.0001
Body temperature (°C)
35.4 ± 0.38
36.2 ± 0.54
36.4 ± 0.87
37.0 ± 1.04
37.6 ± 1.11
38.5 ± 0.66
38.9 ± 0.53
38.14 ± 0.28
37.9 ± 0.19
36.2 ± 0.29
< 0.0001
White blood count (103/μl)
5.5 ± 0.7
-
-
-
-
-
-
-
-
10.9 ± 1.6
0.03
C-reactive protein (mg/l)
1.1 ± 2.4
0.9 ± 1.8
-
-
1.5 ± 2.4
2.2 ± 2.5
1.1 ± 2.3
1.8 ± 2.8
4.8 ± 2.0
60.0 ± 21.5
< 0.0001
Ang-1 (ng/ml)
67.0 ± 20.7
58.2 ± 24.4
-
-
61.2 ± 25.0
54.3 ± 19.5
-
64.9 ± 29.1
60.3 ± 31.4
52.3 ± 21.6
0.053
Ang-2 (ng/ml)
0.57 ± 0.50
0.63 ± 0.20
1.04 ± 0.65
1.63 ± 0.89
2.33 ± 0.69
2.35 ± 1.06
2.42 ± 1.32
2.23 ± 1.18
1.61 ± 1.07
1.51 ± 1.03
< 0.0001
Tie2 (ng/ml)
1.34 ± 0.31
1.23 ± 0.29
1.33 ± 0.32
1.53 ± 0.52
1.23 ± 0.20
1.3 ± 0.16
1.31 ± 0.35
1.4 ± 0.3
1.25 ± 0.32
1.43 ± 0.42
0.085
A non-parametric repeated-measures analysis of variance (Friedman's test) was used to test for significant changes of variables during the time course after LPS challenge (placebo group; n = 6). ANG = angiopoietin; BP = blood pressure; HR = heart rate; LPS = lipopolysaccharide; MAP = mean arterial pressure.
In our cohort of healthy volunteers, neither endogenous sTie2, nor circulating Ang-1 concentrations changed during 24 hours after endotoxin challenge (Table
Angiopoietin-2 release runs in parallel with early pro-inflammatory cytokines and precedes endothelial inflammation after endotoxin challenge
Plasma levels of TNF-alpha were already significantly elevated at 1.5 hours (
Soluble E-selectin appeared in the circulation later than Ang-2 and E-selectin levels were elevated from 4.5 hours until 24 hours (all
Angiopoietin-2 release after endotoxin challenge is attenuated by p38 MAP kinase inhibition
Our previous studies have shown that inhibition of the intracellular p38 MAP kinase attenuated inflammatory responses during human endotoxemia
The AUC of absolute Ang-2 values (ng/ml) were 39.8, 31.0, 32.1, and 17.8 in the placebo and the three interventional groups, respectively. Correspondingly, the AUC of percentage increase in Ang-2 from baseline were 9850, 4765, 3435, and 2567 in the placebo and the three interventional groups, respectively.
Circulating angiopoietin-2 correlates with TNF-alpha levels, soluble E-selectin levels, and the heart rate/mean arterial pressure index
TNF-alpha levels correlated well with Ang-2 at 3.5 (r = 0.44,
Correlation of Ang-2 with TNF-α, E-selectin and heart rate/mean arterial pressure index after LPS challenge in healthy subjects
Correlation of Ang-2 with TNF-α, E-selectin and heart rate/mean arterial pressure index after LPS challenge in healthy subjects. Dot blots showing the correlation between circulating angiopoietin (Ang)-2 and (a) plasma levels of TNF-alpha, (b) plasma levels of the soluble endothelial specific adhesion molecule E-selectin, and (c) the heart rate/mean arterial pressure index (HR/MAP index) at 6.5 hours after lipopolysaccharide (LPS) challenge in 21 subjects (placebo (n = 6), and medication groups: 350 mg (n = 5). 700 mg (n = 6), and 1400 mg (n = 4), respectively). Pearsons correlation coefficient was used after logarithmic transformation of variables (axes denote percentage increase after logarithmic transformation; baseline = 100%).
Excess Ang-2 on admission and increasing Ang-2 level during the early course indicate unfavorable 28-day survival in septic patients
First, circulating Ang-2 on admission was 9.8 ± 3.2 ng/ml in septic patients (n = 21). Regarding the kinetics of Ang-2 during follow-up, mean Ang-2 levels remained unchanged at 24 hours (14.3 ± 4.0 ng/ml) and 72 hours (18.2 ± 6.0 ng/ml) when all patients were analyzed (non-parametric repeated measures ANOVA (Friedman's test);
Time course of Ang-2 in critically ill patients with sepsis
Time course of Ang-2 in critically ill patients with sepsis. Dot blots showing the concentration of angiopoietin (Ang)-2 (ng/ml) in 21 septic on intensive care unit (ICU) admission, 24 hours and 72 hours after admission, respectively. Of note, median Ang-2 levels increased in non-survivors (
Finally, we calculated sensitivity, specificity, and predictive values by 2 × 2 tables including all patients (n = 21) to compare the predictive value between absolute Ang-2 at baseline, absolute Ang-2 at 72 hours, and the decrease/increase of Ang-2 between baseline and during 72 hours. At baseline (admission), a ROC-optimized Ang-2 cut-off value more than 5.9 ng/ml best identified non-survivors with 90% specificity and 81% sensitivity. The positive predictive value was 90% and the negative predictive value 81%. In patients with Ang-2 values more than 5.9 ng/ml, the odds ratio (OR) was 40.5 (95% confidence interval (CI) = 3.7 to 398.1) for death during 28-day follow-up (Fisher exact test
Discussion
The present study dissects the time course of Ang-2 release after experimental LPS administration in healthy subjects. The decisive results are: LPS (4 ng/ml) is a triggering factor for Ang-2 release
Clinical studies of pathophysiological changes during sepsis are potentially confounded by the absence of a well-defined onset time of inflammation, by significant co-morbid conditions, as well as by considerable delays from the presumed initiation of inflammation until study inclusion. Animal studies, although indispensable for investigating early and late events during systemic inflammation, are potentially confounded by major inter-species differences in the sensitivity and immune response to various types of inflammatory stimuli
After LPS infusion, peak Ang-2 levels (2.4 ± 0.5 ng/ml) are four-fold lower than Ang-2 levels in critically ill patients at the ICU (9.8 ± 3.2 ng/ml). Emerging data from our group, as well as a recent study by Siner and colleagues
Ang-2 exhibited a kinetic profile that is similar to the early pro-inflammatory cytokines TNF-alpha, IL-6, and IL-8. In the present study, TNF-alpha level increased somewhat earlier than Ang-2 levels did. As previously shown, the release of TNF-alpha and several other cytokines during human endotoxemia is blocked by p38 MAP kinase inhibition in a dose-dependent manner
Expression of endothelial adhesion molecules such as E-selectin, VCAM-1, and ICAM-1, are a consistent feature of sepsis
Although (circulating) Ang-2 has a significant adverse effect on pulmonary vascular barrier properties in sepsis
Over the past few years, it has been appreciated that multiple components of WPB, such as Ang-2, P-selectin, and IL-8, are co-stored with von Willebrand Factor (vWF), the major constituent of WPBs
As a prepackaged constituent of WPB, it is not surprising that Ang-2 levels on admission are increased in response to early endothelial activation in critically ill patients
Our study has several limitations. The human endotoxin model carries a risk of inappropriate extrapolation from experimental findings to the clinical setting. However, this is the only model that renders an opportunity to study the early mechanisms of endothelial activation during a time course in human subjects. Because vWF (as the major constituent of WPBs) was not determined in this study and citrated plasma samples from the original trial were not available for re-evaluation, we cannot exclude that Ang-2 might have derived from endothelial cells exclusively. At least murine macrophages seem to express smaller quantities of Ang-2, but this has not been tested in experimental sepsis
Conclusions
We could show for the first time that LPS administration is a triggering factor for Ang-2 release in men. Circulating Ang-2 appears in the systemic circulation during experimental human endotoxemia in a distinctive temporal sequence and correlates with TNF-alpha and E-selectin levels. In addition, not only higher baseline Ang-2 concentrations, but also a persistent increase in Ang-2 during the early course identifies septic patients with unfavorable outcomes.
Key messages
• LPS administration is a triggering factor for Ang-2 release in human endotoxemia.
• Circulating Ang-2 appears in the systemic circulation during experimental human endotoxemia in a distinctive temporal sequence and correlates with TNF-alpha and E-selectin levels.
• High Ang-2 concentrations at baseline, as well as a persistent increase in Ang-2 during the early course identifies septic patients with unfavorable outcome.
Abbreviations
ALI: acute lung injury; Ang: angiopoietin; ANOVA: analysis of variance; ARDS: acute respiratory distress syndrome; AUC: area under the curve; CI: confidence interval; CRP: C-reactive protein; ELISA: enzyme linked immuno sorbent assay; ICAM-1: inter-cellular adhesion molecule-1; ICU: intensive care unit; IL: interleukin; ILMA: immunoluminometric sandwich assay; LPS: lipopolysaccharide; MAP: mitogen activated protein; OR: odds ratio; ROC: receiver operator characteristics; TNF-alpha: tumor necrosis factor-alpha; VCAM-1: vascular cell adhesion molecule-1; WPB: Weibel-Palade body.
Competing interests
The authors declare that they have no competing interests.
Authors' contributions
PK had the initial idea, supervised the project, analyzed the data, prepared the figures and wrote the manuscript. MM supervised the project, analyzed the data, made figures and contributed to the manuscript. SD contributed to the idea, identified patients, participated in analysis of the results and contributed to the manuscript. GM participated in analysis of the results and contributed to the manuscript. JB performed the multiplex assays and reviewed the manuscript. AL identified patients, established and performed the immunoassays and reviewed the manuscript. FB collected and analyzed patient data and reviewed the manuscript. HH supervised the project and reviewed the manuscript. JZ designed and supervised the entotoxemia model, enrolled patients, analyzed the data and contributed to the manuscript. PK and MM contributed equally to the work and are both considered first authors.