1Perioperative Outcomes Group and Department of Anesthesiology, 2Department of Surgery, 3Department of Medical Oncology, 4Perioperative Outcomes Group and Department of Health Sciences Research and 5Perioperative Outcomes Group, Mayo Medical School, Rochester, MN, USA*Corresponding author: Department of Anesthesiology, Mayo Clinic, 200 First Street SW, Rochester, MN 55905, USA
An abstract was presented at the American Society of Anesthesiologists meeting in Orlando, Florida, October 20, 1998, and the Midwest Anesthesia Residents Conference in Columbus, Ohio, April 17, 1999.
Accepted for publication: May 2, 2001
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Abstract |
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Br J Anaesth 2001; 87: 44752
Keywords: surgery, carcinoid tumour; complications, cancer; polypeptide, octreotide
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Introduction |
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Methods |
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The perioperative medical, surgical, nursing and anaesthesia records of 119 patients were reviewed to identify preoperative risk factors, intraoperative complications and postoperative complications occurring up to 30 days after surgery according to well-established criteria.24 25
Preoperative information included age, sex, the presence of comorbid disease [cardiovascular, renal, biliary, central nervous system (CNS), respiratory], the presence of carcinoid heart disease as determined by a cardiologist and confirmed by a preoperative echocardiogram, American Society of Anesthesiology physical status, preoperative symptoms of flushing, diarrhoea and/or shortness of breath, preoperative use of bronchodilators, corticosteroids and histamine receptor type 2 antagonists, the preoperative daily dose of octreotide, the dose of octreotide administered in the 8 h preceding the start of anaesthesia, the site of the primary carcinoid tumour, if known, and the most recent preoperative urinary output of 5-hydroxyindoleacetic acid (5-HIAA).
Intraoperative information included the type and duration of anaesthesia, the principal maintenance anaesthetic agent, the use of invasive monitors, the volume and type of i.v. fluids and blood products administered, and the total amount of octreotide administered during anaesthesia. Intraoperative observations included the presence of flushing, urticaria, ventricular dysrhythmia, bronchospasm, acidosis (defined as arterial pH <7.2), lowest PaO2, lowest SpO2, lowest systolic blood pressure (SBP), highest SBP, death, total duration of SBP <80 mm Hg to the nearest 5 min, and treatment with vasopressor(s) (SBP <80 mm Hg for >10 min), and total duration of sustained tachycardia (defined as pulse >120 beats min1) to the nearest 5 min.
Postoperative morbidity occurring within 30 days of the index surgery was identified using criteria developed by Hosking et al.25 and detailed elsewhere.26 Adverse outcomes included myocardial infarction, pulmonary embolism, CNS changes, renal dysfunction, biliary dysfunction, prolonged endotracheal intubation, systemic sepsis and death.
Statistical analysis
Univariate analyses of potential risk factors were performed using the rank sum test for continuous variables and Fishers exact test for categorical variables. Exact confidence intervals for complication frequencies were calculated. In all cases, two-sided tests were performed and P0.05 was used to denote statistical significance.
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Results |
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Of the 15 patients who experienced perioperative complications or death, eight experienced one or more intraoperative complications. Intraoperative complications included flushing in four patients, sustained hypotension in two patients, and bronchospasm, acidosis and ventricular tachycardia in one patient each. There were no intraoperative deaths, episodes of urticaria or ventricular fibrillation.
None of the 45 patients who received octreotide intraoperatively experienced significant intraoperative complications compared with eight of the 73 patients (11%) who did not receive octreotide (P=0.023). Patients who received octreotide intraoperatively and those who did not had similar preoperative characteristics, similar comorbidities including carcinoid heart disease and similar preoperative urinary 5-HIAA output. Octreotide received approval by the Food and Drug Administration (FDA) in 1988, and intraoperative use in this study began in the same year (Fig. 1). We performed an additional analysis restricted to the period during which octreotide was approved for use by the FDA (19881996) to rule out any confounding variables created by possible changes in anaesthetic or surgical management after 1988. This analysis demonstrated that patients receiving octreotide intraoperatively experienced significantly fewer intraoperative complications than patients who did not receive octreotide (0/45 vs 8/60, P=0.010).
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Nine patients experienced one or more postoperative complications. Four patients (3%) developed biliary dysfunction, two patients had renal dysfunction and one patient required prolonged endotracheal intubation. Three patients (2.5%) died postoperatively. Details of the events preceding the three deaths follow.
Death 1
A 67-yr-old woman with severe carcinoid heart disease and a preoperative 5-HIAA output of 218 mg/24 h (1140.1 µmol/24 h) underwent a right hemicolectomy, ileotransverse colostomy, wedge biopsy of the right lobe of the liver and cholecystectomy for carcinoid of the small bowel, hepatic metastasis and cholelithiasis. Surgery was uneventful, and she was haemodynamically stable throughout the procedure. Twelve days later, the ileotransverse colostomy partially dehisced and she underwent resection of a portion of the terminal ileum and proximal transverse colon and an end-to-end ileotransverse colostomy. Four days after surgery, she developed intra-abdominal sepsis. She died 2 days later.
Death 2
A 30-yr-old man with WolffParkinsonWhite ventricular pre-excitation syndrome, severe carcinoid heart disease and a preoperative urinary 5-HIAA output of 495 mg/24 h (2588.9 µmol day1) underwent hepatic artery ligation, resection of a portion of the ileum, and an end-to-end ileo-ileostomy for metastatic carcinoid tumour of the ileum. He was haemodynamically stable throughout the procedure. Postoperatively, he experienced progressive fluid retention (7.5 kg in 9 days) that was refractory to diuresis, as well as dyspnoea and bronchospasm, abdominal distension and lower extremity oedema. Ten days after surgery, he developed shortness of breath, sinus tachycardia and hypotension. These symptoms and signs deteriorated rapidly into electromechanical dissociation from which he could not be resuscitated.
Death 3
A 50-yr-old man was admitted to another hospital for nausea and vomiting, and was found to have abnormal liver function tests. He was transferred to our hospital 8 days later for further evaluation. Computed tomography of the abdomen revealed hepatic lesions consistent with metastases. Preoperative laboratory investigations included a preoperative urinary 5-HIAA output of 837 mg/24 h (4377.5 µmol day1), an aspartate aminotransferase concentration of 89 U litre1, alkaline phosphatase of 590 U litre1, total bilirubin of 5.0 mg dl1 (85.5 µmol litre1) and direct bilirubin of 3.4 mg dl1 (58.1 µmol litre1). A transthoracic echocardiogram demonstrated moderate tricuspid valve regurgitation, but the valves were insufficiently visualized to make a definitive diagnosis of carcinoid heart disease. Five days after admission the patient underwent a retrocolic, isoperistaltic gastrojejunostomy for gastric outlet obstruction secondary to metastatic carcinoid tumour. At surgery, his liver was noted to be 5075% replaced by tumour. Surgery and anaesthesia were uneventful, and he was haemodynamically stable throughout the procedure. He was discharged 8 days after surgery and died 1 week later of unknown cause(s). No autopsy was performed.
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Discussion |
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There are several case series of patients with metastatic carcinoid tumours. Two of these case series predate the availability of octreotide. Kleine et al.20 described the anaesthetic management and intraoperative course of three surgical patients. All three of these patients experienced intraoperative hypertension, one patient also experienced an episode of hypotension and flushing and there were no intraoperative deaths. Miller et al.19 reviewed the intraoperative management of nine patients. Again, no intraoperative deaths were noted. However, one patient had life-threatening haemodynamic instability, four other patients had hypertensive episodes and another developed bronchospasm.
Two more recent case series include reports of patients who received octreotide perioperatively. Ockert and White4 reviewed the perioperative outcomes of six patients who underwent cardiac surgery for carcinoid heart disease. Four patients received octreotide perioperatively. One patient with widespread carcinoid metastases and carcinoid heart disease received octreotide pre- and intraoperatively but still experienced an intraoperative carcinoid crisis. This patient developed a severe coagulopathy after cardiopulmonary bypass and died within 12 h of surgery. The other three patients who received perioperative octreotide did not experience a carcinoid crisis intraoperatively, but one never recovered after the operation and died of respiratory failure and multiple metastases several months later. Veall et al.22 reviewed 22 anaesthetic records of 21 patients with carcinoid syndrome who underwent laparotomy. Eight patients received octreotide preoperatively, and further boluses were administered intraoperatively to an unspecified number of patients. There were no intraoperative deaths, but two patients had sustained tachycardia and another two patients exhibited flushing intraoperatively. It is not stated whether these patients received octreotide intraoperatively. After the introduction of octreotide, intraoperative hypotension was generally reported to be less severe and was rapidly responsive to additional i.v. boluses of octreotide.
Urinary 5-HIAA appears to be a good biological marker for the assessment of carcinoid tumour activity23 and its association with perioperative morbidity. We found that patients who had higher preoperative urinary 5-HIAA output were more likely to develop perioperative complications, including death. Similarly, Connolly et al.27 reviewed the perioperative courses of 26 patients who underwent cardiac surgery for carcinoid heart disease and found that high preoperative urinary 5-HIAA output predicted decreased survival after operation. Their finding is not surprising because involvement of the heart disease is typically a late manifestation in the course of carcinoid disease. Pellika et al.28 found that the mean output of urinary 5-HIAA among patients with carcinoid tumours was higher in 74 patients with carcinoid heart disease than in 51 patients without carcinoid heart disease (270 vs 131 mg/24 h, P<0.001) (1412.1 vs 685.1 µmol day1). However, an association between high preoperative urinary 5-HIAA output and perioperative morbidity was not detected in the series of 21 patients reviewed by Veall et al.22 These authors noted that preoperative urinary 5-HIAA output was a poor predictor of perioperative cardiovascular stability in their patient population. In fact, severe hypotension occurred in one patient with a preoperative urinary 5-HIAA output of 11.8 mg/24 h (62 µmol day1).
Two of the three postoperative deaths in our study occurred in patients with severe carcinoid heart disease. The other death occurred in a patient with tricuspid regurgitation, whose valves were poorly visualized on transthoracic echocardiogram and therefore a definitive diagnosis of carcinoid heart disease could not be made. Patients with carcinoid heart disease usually experience symptoms of carcinoid syndrome (i.e. flushing, diarrhoea and shortness of breath) along with the symptoms of right-sided heart failure because of carcinoid-induced tricuspid or pulmonary valve involvement. Carcinoid heart disease and the associated right heart failure are a major cause of morbidity and mortality in these patients.27
Limitations of our study include the reliability of data notation on the medical record. However, we used rigorous definitions and abstracted only major events to increase our chances of capturing information reliably. There is clearly a referral bias at this tertiary care centre in that the patients in this study are not representative of any general population. It is quite likely that referred patients have more severe carcinoid disease, more comorbidities, and require more extensive surgery than those from our local population. We did not assess geographical characteristics in this study. The retrospective nature of this study precludes discovery of the reasons for which octreotide was administered before or after operation. It also prevents us from evaluating any causal relationship between medications or risk factors and perioperative complications. Specifically, this study was not able to evaluate the efficacy of intraoperative octreotide therapy to prevent intraoperative carcinoid crises. Additionally, although this investigation identified some characteristics that were associated with perioperative complications, the interpretation of no association between other patient or procedural characteristics and perioperative complications should be made with caution. In general, with only 15 of 119 patients experiencing complications, an analysis of potential risk factors has statistical power of less than 55% to detect a risk factor with a corresponding odds ratio of 3.0.
Our findings suggest that most people with metastatic carcinoid tumours can undergo intra-abdominal surgery safely. In our patient population, no intraoperative complications occurred in those who received octreotide intraoperatively. Overall, perioperative complications and death were strongly associated with the preoperative presence of carcinoid heart disease and higher elevated urinary 5-HIAA output.
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Acknowledgements |
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References |
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