Case report
A 53-year-old woman was transferred from another hospital with progressive jaundice and lower extremity edema that had lasted for 6 weeks. She was previously treated for 2 weeks with prednisolone for suspected alcoholic hepatitis (AH). She had a long history of heavy alcohol use and her last drink was 4 weeks prior to admission. On arrival, her temperature was 96.5° F, pulse was 97/min, respiratory rate was 16/min, and blood pressure was 118/82. Physical examination was significant for icteric skin and sclera, non-tender obese abdomen with hepatomegaly, and lower extremity pitting edema. Laboratory profile showed serum bilirubin of 22.2 mg/dL, direct bilirubin of 14.8 mg/dL, alanine aminotransferase (ALT) of 85 U/L, aspartate aminotransferase (AST) of 242 U/L, alkaline phosphatase ALP 805 U/L, gamma-glutamyl transferase (GGT) of 2582 U/L, white blood cell count (WBC) of 23.8 µL, and ammonia of 89 mg/dL. Liver enzymes were elevated from previous lab work done 2 weeks prior (AST of 196, ALT of 34, ALP of 338).
The patient was not taking any medications known to cause cholestasis. Her medications on admission included furosemide, spironolactone, prednisolone, and lactulose. Her Lille score was 0.9, suggesting poor response to steroids, and prednisolone was discontinued. Infectious studies were negative, including urine cultures, blood cultures, chest radiograph, and ascitic fluid analysis. Acute viral hepatitis (A, B, and C) was ruled out by respective serological testing for each. Anti-nuclear antibody, anti-mitochondrial antibody and anti-smooth muscle antibody tests were negative. Acetaminophen and salicylate levels were undetectable.
Abdominal ultrasound showed an enlarged (24.5 cm) steatotic liver, cholelithiasis, and a 4-mm common bile duct. Magnetic resonance cholangiopancreatography confirmed liver enlargement without intra or extra-hepatic biliary dilation. Given the presence of cholelithiasis and jaundice, endoscopic ultrasound was performed and ruled out choledocholithiasis or extrahepatic bile duct obstruction. Trans-jugular liver biopsy performed 1 week after presentation showed changes consistent with severe AH, including neutrophilic lobular infiltration, Mallory hyaline, ballooning degeneration of hepatocytes, and cholestasis of ductules and canaliculi. Trichrome stain confirmed presence of cirrhosis (Fig. 1). The patient’s Maddrey’s discriminant function of 35 and model for end-stage liver disease score of 22 were consistent with severe AH.
The patient was discharged to home with outpatient follow-up scheduled at 4 days. Two days after discharge, the patient was readmitted with altered mental status. She had severe metabolic acidosis (lactic acid 18 mg/dL), WBC of 22.2 µL, and ammonia level of 686 mg/dL. Serum bilirubin was 10.2 mg/dL, which represented an improvement from 15.6 at time of discharge. Urine culture was positive for extended-spectrum beta-lactamase (ESBL)-producing E. coli and blood cultures for streptococcus viridians. Unfortunately, despite aggressive resuscitative efforts, she passed away within 24 hours of re-admission.
Discussion
This case represents an atypical presentation of AH with marked elevation of ALP. AH is clinically diagnosed by the presence of jaundice, serum bilirubin of > 3 mg/dL, AST to ALT ratio of > 1.5 with elevated levels but not exceeding 400 IU/L, heavy alcohol use (typically for > 5 years) until at least 6 weeks prior to presentation, and exclusion of other causes of liver disease.1 ALP is elevated in AH patients, with levels usually within 2–3 times the upper limit of normal (ULN), even among non-survivors.2 ALP and GGT levels in our patient were 805 U/L (over 7 times ULN of 117 at our center) and 2582 IU (over 40 times ULN of 65 at our center), respectively. Mild to moderate elevation of ALP in AH patients has been well documented in the literature, but very high levels of ALP are rarely reported. In 1978, Perrillo and his colleagues3 published a case series of 20 alcoholic patients who presented with ALP elevations of approximately 4 times the ULN (mean: 582 and SD: 37 IU/L). Given this atypical presentation of marked elevation of ALP and GGT, diligent work-up was obtained to exclude biliary obstruction, and trans-jugular liver biopsy was performed to confirm the diagnosis of AH.
The patient’s presentation was most likely secondary to infection in the setting of severe AH. While the initial infectious workup was negative, cultures obtained on re-admission showed Gram-positive bacteremia and an ESBL-producing urinary tract infection. The principal mechanisms of cholestasis caused by infection include disruption of bile flow and impairment in bilirubin metabolism.4 Infections are common in AH patients with prevalence of 12–26%, and have negative impact on short-term survival, especially among non-responders to corticosteroids, as in our patient.5 This raises important issues regarding the protocol for infection surveillance in AH patients and the clinically unmet need of biomarkers for early diagnosis of infections in AH.
Our patient had features of systemic inflammatory response syndrome (SIRS). However, SIRS is present in about 60% of AH patients but only 20–30% of patients are diagnosed with infection.6 Potential biomarkers are procalcitonin, lipopolysaccharide, and bacterial DNA and need to be tested in well-designed clinical trials before recommending their routine use in clinical practice. ALP level and cholestasis on liver biopsy are associated with poor patient outcome.5 In a study on 116 AH patients, ALP > 1.5 ULN was independently associated with poor 90-day survival, with mean ALP of 169 IU/L in survivors compared to 236 IU/L in non-survivors.7 However, whether the presence of cholestasis and elevated ALP indicate infection risk remains a testable hypothesis.
Conclusions
In summary, we describe an atypical presentation of markedly elevated ALP in a patient diagnosed with severe AH. Clinicians should be aware of this potential presentation of this common liver disease, remain vigilant for infections in these patients, and utilize liver biopsy early when diagnosis remains uncertain.
Abbreviations
- AH:
alcoholic hepatitis
- ALP:
alkaline phosphatase
- ALT:
alanine aminotransferase
- AST:
aspartate aminotransferase
- ESBL:
extended-spectrum beta-lactamase
- GGT:
gamma-glutamyl transferase
- ULN:
upper limit of normal
- WBC:
white blood cell
Declarations
Conflict of interest
The authors have no conflict of interests related to this publication.
Authors’ contributions
Review of literature and drafting of manuscript (PA), critical revision of the manuscript (KR, AKS).