A Case of Reye Syndrome Caused by Influenza A Virus

CASE REPORT

A 2-year-old male with no significant medical or family history presented to the emergency department (ED) after he was found unresponsive with vomitus in his mouth. He had influenza-like symptoms including cough, rhinorrhea, diarrhea, vomiting, and fatigue without fever 3 days prior to presentation. His parents gave him acetaminophen twice daily for symptom control. On initial physical examination in the ED, the patient had a Glasgow Coma Scale score of 8 and was somnolent but arousable, withdrawing to pain, perfusing well, spontaneously breathing, and had bilateral clonus. Pupils were equal size and constricted with light. Vital signs were normal for his age. Rapid viral testing was positive for influenza A virus. Significant laboratory results included anemia (hemoglobin 9.2 g/dL), hypernatremia (serum sodium 152 mmol/L), transaminitis (aspartate aminotransferase [AST] 3,460 U/L and alanine aminotransferase [ALT] 1,956 U/L), hyperbilirubinemia (total bilirubin 2.4 mg/dL, direct bilirubin 1.9 mg/dL), elevated international normalized ratio (INR 4.7), hyperammonemia (serum ammonia 96 μmol/L), lactic acidosis (serum lactic acid 3.2 mmol/L), azotemia (blood urea nitrogen 50 mg/dL), hypercreatinemia (serum creatinine 0.92 mg/dL), elevated creatine phosphokinase (544 U/L), elevated procalcitonin (25.9 ng/mL), elevated C-reactive protein (1.44 mg/dL), and hypoglycemia (serum glucose 5 mg/dL). Gamma-glutamyltransferase was normal (12 U/L); salicylate, ethanol, and urodynamic studies were negative. The patient was admitted to the hospital. His initial serum acetaminophen level of 30 mcg/mL had decreased to 8 mcg/mL at admission.

On day 1 of his hospitalization, the patient’s liver function deteriorated; AST increased to >20,000 U/L, ALT to 9,509 U/L, and ammonia to 180 μmol/L. Two days after admission, he was transferred to the pediatric intensive care unit for hepatic failure. He became delirious, agitated, and combative and had unintelligible speech. He was intubated and placed on mechanical ventilation for grade 3 hepatic encephalopathy. All tests in an extensive diagnostic evaluation, including testing for autoimmune, inflammatory, infective, toxicologic, metabolic, hematologic, and oncologic etiologies, were negative. Urinalysis on the fourth day of admission revealed proteinuria (urine protein 100 mg/dL) indicative of rhabdomyolysis, but the urine was negative for urobilinogen and nitrites.

Because of the patient’s liver failure and positive result for influenza A, Reye syndrome was the leading differential. Liver biopsy revealed central hepatic venous collapse with surrounding microvesicular steatosis of the hepatocytes consistent with Reye syndrome (Figures 1 and 2).

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Figure 1. Prominent microvesicular steatosis with zone 3 hepatocyte dropout and paucity of inflammatory cells (magnification 20 × ).

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Figure 2. A closer look at microvesicular steatosis (magnification 40 × ).

In addition to supportive care, the patient was treated with lactulose every 6 hours and rifaximin 10 mg/kg twice daily to lower serum ammonia levels. This treatment continued for 8 days. The patient was extubated on day 7. His liver function gradually improved with supportive care, fresh frozen plasma, and vitamin K 10 mg/kg as needed. His liver enzymes trended down from AST 4,986 U/L and ALT 5,841 U/L on day 3, to AST 421 U/L and ALT 1,744 U/L on day 6, and to AST 53 U/L and ALT 208 U/L on day 17 of his hospitalization. His INR trended down from 3.2 on day 2, to 1.9 on day 5, and to 1.2 on day 10. He developed hypertension thought to be caused by acute kidney injury secondary to rhabdomyolysis. Maximum blood pressure was 169/98 mmHg on day 14, and he was treated with labetalol 2 mg/kg/day initially. He remained on labetalol through discharge with good response. His total duration of hospital stay was 17 days, and he was discharged home. On follow-up 4 months following discharge, the patient’s guardians reported that he was achieving normal developmental milestones.