Introduction
Cardiac surgery with extra-corporal circulation (ECC) is associated with a systemic inflammatory reaction that comprises the release of pro- and anti-inflammatory mediators [
1]. The inflammatory balance is thought to condition postoperative morbidity and mortality [
2] and is influenced by numerous patient dependent and independent variables such as genetic predisposition, pre-operative hypoxemia or heart failure, complexity of surgery that impacts the duration and the quality of the whole management of ECC in terms of flow pattern, blood- and patient temperature, duration of myocardial ischemia, and peri-operative medication [
3].
Besides circulating immune competent blood cells, other cell types such as endothelial-, myocardial-, and hepatic cells synthetize inflammatory mediators upon stimulation [
4‐
7] and contribute to the inflammatory response to cardiac surgery. Cytokine signaling involves not only the classical infectious- and inflammatory- but also mechanical stress pathways that share common transcription pathways such as that of nuclear factor kappa B (NFκB) and activating protein (AP)-1 [
8].
Hence, hemodynamic load that initiates mechanical stress of endothelial- or myocardial cells stimulates up-regulation of inflammatory genes [
5,
6,
9]. In addition, systemic and pulmonary endothelial cells sense various flow patterns and respond via the activation pathway of NFκB [
10]. Therefore, the characteristics of myocardial overload and of pulmonary flow in a patient before or immediately after the operation are expected to influence the inflammatory response to cardiac surgery. With this respect, hemodynamics after total cavo-pulmonary connection created for UVP-palliation that is characterized by at least a non-pulsatile pulmonary flow and increased central venous pressure with systemic and particularly hepatic vein congestion has the potential to modulate the peri-operative innate immune response [
11]. This latter is complex and comprises the interplay of members of families of pro- and anti-inflammatory cytokines. Classical representative of pro-inflammatory cytokines are TNF-α and IL-12 [
12,
13]. IL-6 has early pro- and later anti-inflammatory properties and is the main inductor of the acute phase reaction [
14] whereas IL-10 is the major monocyte deactivating anti-inflammatory cytokine that contributes to termination of inflammation [
15]. Given the inhibitory effect of IL-10 on the synthesis of pro-inflammatory cytokines, the inverse ratio between its levels and those of TNF-α are commonly used to reflect the inflammatory balance in diverse clinical situations [
16]
In this study, we aimed to test the hypothesis that children undergoing UVP would show a different inflammatory balance than patients undergoing BVR. For this purpose, we analyzed data of a historical cohort of patients (surgery 1995–2000). We are aware that nowadays UVP is performed without cardioplegic arrest. Nevertheless, this similar surgical approach as well as a relatively homogenous hemodynamic situation preoperatively enabled us to directly compare the inflammatory response in patients undergoing UVP or BVR.
Methods
Patients
After approval by our local Human Ethical Committee and informed consent of the parents, 20 children aged 15–176 months, median 39.5 months with complex cardiac malformations were included in this prospective study. Twelve patients underwent UVP, 8 BVR. Characteristics of the patients groups are summarized in Table
1.
Table 1
Epidemiological and operative variables in children after uni-ventricular palliation or bi-ventricular repair
n | 12 | 8 | |
Male/female (n) | 7/5 | 7/1 | NS |
Age at operation (months) | 39.5 (88.2) | 39.5 (62.5) | NS |
SaO2 (%) | 78 (5.2) | 84 (18.3) | NS |
Cardiac malformation | SV (n = 7) TA (n = 3) Other (n = 2) | TOF (n = 5) PA-VSD (n = 3) | |
Previous palliation | AP shunt n = 4 PAB n = 6 | AP shunt n = 7 | |
Duration of ECC (min) | 89.5 (82.8) | 87 (47.8) | NS |
Duration of aortic clamping (min) | 69.8 (61.5) | 67 (25.5) | NS |
Water balance during ECC (ml) | 135 (370) | 162.5 (481) | NS |
Operation and post-operative care
In all cases, conventional general anesthesia consisted of isoflurane and sufentanyl. Dexamethasone (1 mg/m2 body surface area) was given before sternotomy. Perioperative antibiotic prophylaxis was carried out with cefuroxime. After institution of moderate hypothermic low-flow cardio-pulmonary bypass (CPB), the aorta was cross-clamped and cardiac arrest was instituted by intra-aortal injection of 4 °C cold cardioplegic solution (Bretschneider, 30 ml/kg body weight), which was re-aspirated in the right atrium. At the end of the intra-cardiac operative procedure, the patient was weaned from CPB under progressive re-warming. Epicardiac pace-maker leads and pericardial- and mediastinal drains were placed before chest closure.
Arterial blood pressure and central venous pressure were continuously monitored via an arterial- and a central venous line, respectively.
Inotropic support consisted of dobutamine given to maintain a normal mean arterial blood pressure for age and volume therapy by injections of crystalloid solutions, if requested.
The patient was transported on the intensive care unit where the weaning from the artificial ventilation was begun as early as possible. The ratio between arterial partial pressure of oxygen (PaO2) and fraction of inspired oxygen (FiO2) was used to assess oxygenation. Diuresis was continuously monitored via a bladder catheter as was water balance.
Routinely performed laboratory investigations included at least the determination of blood gases, blood concentration of lactate, glycemia, complete blood count, serum creatinine, aspartate aminotransferase (AST), coagulation parameters, and were measured at least 4- and 24 h post-operatively
Blood samples
Venous blood was collected in EDTA tubes before the operation, 10 min after beginning of ECC, after protamine administration, 4 h post-operatively (4 h po), 1-, 2-, 3-, and 10 days after the operation (POD -1, -2, -3, and -10).
The samples were immediately centrifuged for 3 min (3000 rpm) and the plasma was stored at − 80 °C until analysis.
Cytokine determination
TNF-α, IL-6, IL-10, and IL-12 were measured by enzyme amplified sensitivity immunoassay (EASIA, BioSource®, Belgium) according to the manufacturer’s recommendation.
Procalcitonin (PCT)
PCT was determined using a specific immunoluminometric assay (Lumitest PCT, Brahms Diagnostica GmbH, Berlin, Germany). The detection limit of the method is 0.1 ng/ml. Normal values for healthy adults are < 0.1 ng/ml.
Statistical analysis
Results are expressed by median and interquartile range (IQR) assuming not normal distribution of the data. For intergroup comparison of independent clinical and of biologic variables at specific sample times, the nonparametric Mann-Whitney U was used and the Wilcoxon test for the comparison of dependent variables when required. The Spearman rank correlation coefficient was assessed for correlation of independent parameters. P values < 0.05 were considered significant. Alpha adjustment for multiple comparisons was performed according to Bonferroni-Holm.
Discussion
Our results confirm that cardiac surgery in children induces a systemic release of the pro- and anti-inflammatory cytokines TNF-α, IL-6, IL-10, and IL-12 that persists at least up to POD 5, and that the importance of the inflammatory response is well reflected by the early post-operative PCT levels.
TNF-α is an early pro-inflammatory cytokine that has also a role in the maintenance of homeostasis [
12]. It induces among others IL-6 [
17]. TNF-α and IL-6 are implicated in the pathophysiology of heart failure and of pulmonary hypertension [
18]. IL-6 helps terminating inflammation via the induction of C-reactive protein in the liver and via the induction of the monocyte deactivating cytokine IL-10 [
15]. The liver is an important source of IL-10 during cardiac surgery, as we showed previously [
7]. IL-10 inhibits the synthesis of all pro-inflammatory cytokines via the activation of the suppressor of cytokine signaling (SOCS) [
19]. SOCS in turn is modulated by mechanical stress as it has been shown in human endothelial cells [
20].
IL-12 is a pro-inflammatory cytokine that is produced by antigen presenting cells such as dendritic cells and macrophages. It regulates interferon-γ (INFγ) production by Th1 lymphocytes [
13]. In adults and children undergoing cardiac surgery, decreased ex vivo IL-12 production has been demonstrated [
21,
22], thus favoring anti-inflammatory balance [
23].
In the present series, upon connection with the ECC circuit, the concentrations of TNF-α and IL-12 fall significantly. This decrease may be the result of the combined effects of dilution and corticosteroids given before the operation [
24]. Both pro-inflammatory cytokines showed a similar course with a secondary significant increase of their blood concentrations during ECC and a peak value measured 4 h po, reflecting the pro-inflammatory effect of cardiac surgery [
3]. The correlations between TNF-α levels at the end of ECC and the volume of water retention during ECC and the oxygenation index on POD 1, respectively, confirm the harmful impact of inflammation on endothelial- and organ function [
3]. The second decrease of TNF-α- and IL-12 concentrations with a nadir on POD 3 reflects the counteracting effect of the anti-inflammatory response [
25]. This latter was objectivized in this series by an early and significant increase of IL-10 blood concentrations reaching their peak value at the end of ECC. Interestingly, the importance of the early release of IL-10 was associated with higher mean arterial blood pressure in the early post-operative period, reflecting the clinical relevance of the anti-inflammatory response during cardiac surgery.
IL-6 showed a similar course to IL-10. IL-6 has early pro- and later anti-inflammatory properties as well and its blood levels usually reflect the amount of systemic inflammation [
26]. In this series, its early release after connection to ECC was associated with lower CVP, confirming the role of inflammation in the pathophysiology of capillary leakage during cardiac surgery [
27].
The comparison of the time course of TNF-α and IL-12 blood concentrations on the one hand and of IL-6 and IL-10 on the other hand is suggestive for the interplay between pro- and anti-inflammatory signals during and after cardiac surgery [
1]. This is supported by the significant correlations between TNF-α and IL-10 concentrations we observed in the early post-operative period.
The TNF-α/IL-10 ratio can be considered a marker of the inflammatory balance [
28]. In this series, higher ratio correlated with lower water balance during CPB, confirming again the role of inflammation in capillary leakage during cardiac surgery.
The main objective of this study was to test the hypothesis that patients with UVP circulation would respond differently to cardiac surgery in terms of systemic inflammation than patients undergoing BVR. Our results allow suggesting such a differential response. Indeed, patients after UVP showed significantly lower concentrations of TNF-α and IL-12 with higher IL-6 blood levels and lower TNF-α/IL-10-ratio in the early post-operative period than BVR patients. This is indicative for a shift of the inflammatory balance towards anti-inflammation in patients with UVP.
The systemic inflammatory reaction elicited by cardiac surgery is complex and influenced by numerous patient-dependent or patient-independent variables [
3]. With this respect, intra- and post-operative hemodynamics is potentially an important influencing factor [
29]. Patients with UVP have as main hemodynamic characteristics high CVP with distension of the systemic venous system and non-pulsatile arterial pulmonary blood flow. Our results showing higher CVP in the early po period in UVP than BVR patients are concordant with this.
Mechanical stretch encountered in arterial and venous vessels under normal or pathological conditions have a direct impact on endothelial cell function throughout the activation of several transcription pathways such as that of NFκB and AP-1 that are common to the inflammation pathways [
30,
31].
Thus, high pulsatility flow due to vascular stiffening has been shown to induce significant acute and sustained endothelial inflammation mediated by the activation of NFκB whereas low pulsatility flow was associated with only minor and transient inflammation [
32]. Not only flow pulsatility but also the helical flow structure initiates inflammatory signals in endothelial cells via NFκB activation, leading to the downstream synthesis of IL-1β, TNF-α, IL-6, and INFγ [
9].
Helical flow structure has been demonstrated in the right artery after cavo-pulmonary connection [
33] but whether it influences local or the systemic inflammatory pathways has not been investigated yet.
Besides the impact of flow pattern on the endothelial inflammatory signals, mechanical stretch of myocardial cells due to hemodynamic overload of cardiac cavities induces an intra-myocardial expression of pro- and anti-inflammatory cytokines, as we showed previously in children with congenital cardiac defect [
5]. These inflammatory mediators are released into the circulation [
34] and may participate to the inflammatory response to cardiac surgery and influence post-operative outcome.
Limitations
The small patient number that did not allow to test the possible relationship between hemodynamics and markers of inflammation during and after the operation is the main limitation of our study.
It is of note that surgery for the patients described in our study was performed in the years 1995 to 2000. Surgical techniques have been substantially modified and evolved in the meantime. But it was the relatively homogenous group of patients (with pulsatile flow characteristics in the pulmonary circulation preoperatively in all patients) that enabled us to compare the differential cytokine response between patient undergoing UVP or BVR.
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