Late pharmacologic conditioning with volatile anesthetics after cardiac surgery

This is a prospective randomized parallel group trial comparing postoperative propofol with sevoflurane sedation in the ICU after on-pump cardiac surgery. All patients between 18 and 90 years of age, scheduled for elective cardiac surgery requiring the use of ECC at the University Hospital Zurich, Switzerland, were eligible. Exclusion criteria were poor cardiac baseline function, defined as an ejection fraction of < 30%, significant coronary impairment (CCS ≥ 3 or myocardial infarction within 7 days before the surgery date), emergency procedures, previous cardiac surgery, chronic pulmonary disease (FEV₁ < 80% or FEV₁/FVC < 70% of predicted value), renal dysfunction (creatinine clearance, < 60 ml/min), insulin-dependent diabetes mellitus, pregnancy, and current steroid treatment.

Randomization was computer generated with prestratification for the following surgery groups: (a) aortic valve surgery, (b) mitral valve surgery, and (c) combined procedures with coronary artery bypass grafting (CABG) or replacement of the ascending aorta. The envelope was opened by an investigator at the end of the case. Anesthesiologists and surgeons were blinded to the intervention.

The local ethics committee (Ethic committee, Kantonale Ethikkommission, University Hospital Zurich, Switzerland) approved the trial (StV 5-2007). The study was registered in ClinicalTrials.gov as NCT00924222. Written informed consent was obtained from all study subjects.

Preoperatively patients underwent routine clinical and laboratory examinations. Before surgery, they received oral midazolam at the clinical discretion of the anesthesiologist. For the surgical procedure, patients were monitored in a standard fashion with a five-lead electrocardiogram, pulse oximetry, invasive blood pressure measurement, central venous pressure measurement, bispectral index (BIS), and transesophageal echocardiography. Direct measurement of pulmonary artery pressure was used in more complex cases. The cardiopulmonary bypass (CPB) technique was nonpulsatile, using a roller pump. Active cooling was performed, aiming at temperatures of 32°C to 34°C. Crystalloid cardioplegia was used without hot shot. All patients received general anesthesia with a target-controlled infusion of propofol, fentanyl boluses, plus remifentanil as a continuous infusion. Muscular relaxation was achieved with pancuronium at the induction of anesthesia. Volatile anesthetics were not applied to the patient in the operating room at all. After surgery, patients were transferred to the ICU under continuous analgosedation with propofol and remifentanil.

Patients in the control group received propofol titrated by the critical care team within a range of 0.5 to 4.0 mg/kg BW per hour to achieve continuous sedation (total intravenous application, no target-controlled infusion). Propofol was started at a rate of 2 mg/kg/h and adjusted according to the sedation score and hemodynamics. Remifentanil at a dose of 0.05 to 0.2 μg/kg BW per minute was added as needed to achieve analgesia. In the treatment group, patients were switched to an inhalational sedation regimen with sevoflurane immediately after arrival at the ICU. For this purpose, sevoflurane (Sevorane; Abbot, Abbot Park, IL, USA) was applied via the AnaConDa system at a starting dose of an age-adjusted minimum alveolar concentration (MAC) of 0.5 [16], and was titrated to balance sedation. The end-tidal concentration of sevoflurane was measured by using a Dräger Scio gas module (Dräger Medical, Lübeck, Germany). Remifentanil was applied to patients in the sevoflurane arm at the same does as in the propofol group (0.05 to 0.2 μg/kg/BW). The minimal duration of sedation was 4 hours. During sedation, the patients were monitored with five-lead electrocardiogram, pulse oximetry, invasive blood pressure measurement, and central venous pressure measurement. The AnaConDa module was incorporated in the respiratory circuit of all patients in both groups to control for any unknown effects of the system itself. A CONTRAfluran active charcoal filter (ZeoSys GmbH, Berlin, Germany) was used on the expiratory valve of the ventilator to minimize environmental contamination with sevoflurane. For mechanical ventilation, the ventilator Evita XL (Dräger, Lübeck, Germany) was used in biphasic positive airway pressure (BiPAP) mode with a first positive endexpiratory pressure (PEEP) of 6 cm H₂O and tidal volumes of 6 to 9 ml/kg. The settings were adjusted to maintain a p_aCO₂ of 5.0 to 6.0 kPa. The F_iO₂ was set to reach an age-adapted p_aO₂ between 8.5 and 10 kPa. Once the patient fulfilled extubation criteria (adequate cardiac function, hemodynamic stability, no coagulopathy, no bleeding, adequate pulmonary function and respiratory effort, including normal postoperative chest radiograph and sufficient blood gas analysis, as judged by the intensivist), the application of propofol or sevoflurane was stopped.

Any postoperative nausea and vomiting (PONV) was treated according to the following scheme: (a) topisetron, 2 mg, plus droperidol, 0.5 mg, intravenously (iv) applied; (b) repeated droperidol, 0.5 mg, iv; (c) meclozin/pyridoxin/caffeine (50/50/20 mg) suppository; and (d) metoclopramide, 10 mg iv. Steroids and propofol were not used for this purpose.

The primary outcome was defined as cardiac injury on the first postoperative day (POD1) measured by troponin T 12 to 18 hours after surgery. Additional biochemical outcomes were creatine kinase (CK), myocardium-specific creatine kinase (CK-MB), and myoglobin. All laboratory values were determined on arrival in the ICU (considered baseline values), 4 hours after initiating postoperative sedation in the ICU, and in the morning of POD1. The following normal ranges are accepted for the different parameters: troponin, < 0.014 μg/L; CK, < 190 U/L; CK-MB, 28 to 72 U/L; and myoglobin, < 24 μg/L.

Secondary end points included oxygenation index (p_aO₂/F_iO₂) after 4 hours of sedation before extubation and at POD1, incidence of postoperative pulmonary complications (any of the following: temperature > 38.5°C plus productive cough, radiologic signs of pneumonia or pathologic organisms in Gram stain or culture; initiation of antimicrobial therapy; need for reintubation) during hospitalization, duration of ICU and hospital stay, and the need for antiemetics.

To control for possible remaining confounders, the following parameters were additionally recorded: ECC time, aortic cross-clamp (ACC) time, and administration of blood products.

The study was powered to detect a difference of 0.3 U/L in troponin on POD1 between the two groups with a standard deviation of 0.5 U/L, a β of 0.8, and an α of 0.05. The expected number in each group was 44.

The data analyst was masked for group assignment when performing the statistical analyses, and the randomization code was broken only after the analyses were completed. A per-protocol analysis was performed: we analyzed all patients according to the randomization and whether they received the randomly assigned intervention. We did not include patients in the analyses who were extubated early and who could not be sedated appropriately, because we did not collect outcome data for these patients.