Acute intraoperative tumour lysis syndrome

Abstract

To the Editor, The patient provided written informed consent for the clinical report that follows. A previously healthy 54-yr-old woman presented to hospital with a two-week history of fatigue, dyspnea, and spontaneous bruising. Investigations revealed a white cell count of 3.9 9 10 L with blast cells, hemoglobin of 43 g L, and a platelet count of 47 9 10 L. A diagnosis of acute myeloid leukemia was made, and the patient was started on cytarabine and hydroxyurea. The next day, she developed left-sided weakness and confusion. Her platelet count had fallen to 10 9 10 L, and computed tomography showed a large right tempo-parietal intracerebral hemorrhage with midline shift. She was transferred to our tertiary neurosurgical centre for emergency craniotomy and evacuation of the hematoma. Upon admission to the intensive care unit (ICU), the patient had a Glasgow Coma Scale of 6, and her trachea was intubated after administering propofol and rocuronium. Preoperative laboratory investigations included arterial pH 7.42, PaCO2 32 mmHg, PaO2 69 mmHg, Hb 58 g L, platelets 91 9 10 L, Na 132 mmoL L, K 3.1 mmoL L, and creatinine of 131 lmoL L. To treat hypokalemia, potassium chloride 10 mmoL iv was administered by the ICU staff prior to transferring the patient to the operating room (OR). In the OR, the patient received two units of platelets prior to skin incision and four units of blood over the next 30 min. Approximately 40 min after skin incision, the patient’s heart rate (HR) fell abruptly from 90 to 50 beats min. The P waves remained visible on the electrocardiogram (ECG), but gradual widening of the QRS complex was observed (Figure). Her blood pressure (BP) decreased from 110/70 to 80/50 mmHg. Ephedrine 10 mg iv was given with a transient increase in HR and BP. The QRS complex continued to widen, P waves disappeared, and the patient’s BP fell to 60/40 mmHg. Intravenous boluses of atropine (total 0.8 mg), phenylephrine (total 1 mg), and ephedrine (total 45 mg) were given, but again with only transient effect. At this point, the OR was notified that the serum potassium on the arterial blood gas (ABG) was 7.4 mmoL L. We immediately treated the hyperkalemia with 10 mL of 10% calcium chloride iv, 10 units of insulin iv with an intravenous glucose bolus, and furosemide 20 mg iv. Within minutes of calcium administration, the QRS complex began to narrow and both BP and HR increased. An intravenous infusion of dopamine was started at 5-10 ug kg hr and titrated to BP. Serial intraoperative ABGs showed a progressive decline in serum potassium over 50 min (from 7.4 to 6.9 to 6.4 mmoL L). This decline correlated with hemodynamic stabilization and the return of P waves and a normal QRS width on the ECG. Review of the patient’s laboratory investigations showed concomitant hyperuricemia (706 lmoL L), hyperphosphatemia (1.79 mmoL L), and hypocalcemia (0.88 mmoL L), suggesting acute tumour lysis syndrome (TLS) as the cause of hyperkalemia. In this patient, TLS was heralded by acute bradycardia, loss of P waves, and a widened QRS complex, which are all consistent with hyperkalemia. The differential diagnosis of the arrhythmia, apart from electrolyte abnormalities, included structural heart disease, myocardial ischemia, hypoxemia, hyper/hypocarbia, acid/base disturbances, and hypothermia, none of which was evident from the patient’s history or clinical condition at the time. The finding of acute hyperkalemia was unexpected; succinylcholine had not been used, and in our opinion, the administration of only F. Alam, MD K. J. Chin, FANZCA (&) Toronto Western Hospital, Toronto, ON, Canada e-mail: gasgenie@yahoo.co.uk