Acute Liver Failure in Infants and Young Children in a Specialized Pediatric Liver Centre in India

Seema Alam; Bikrant Bihari Lal; Rajeev Khanna; Vikrant Sood; Dinesh Rawat

doi:10.1007/s12098-014-1638-6

Acute Liver Failure in Infants and Young Children in a Specialized Pediatric Liver Centre in India

Indian J Pediatr. 2015 Oct;82(10):879-83. doi: 10.1007/s12098-014-1638-6. Epub 2015 Jan 6.

Authors

Seema Alam¹, Bikrant Bihari Lal², Rajeev Khanna², Vikrant Sood², Dinesh Rawat²

Affiliations

¹ Department of Pediatric Hepatology, Institute of Liver and Biliary Sciences, D1 Vasant Kunj, New Delhi, 110070, India. [email protected].
² Department of Pediatric Hepatology, Institute of Liver and Biliary Sciences, D1 Vasant Kunj, New Delhi, 110070, India.

PMID: 25557177
DOI: 10.1007/s12098-014-1638-6

Abstract

Objective: To study the etiological spectrum of acute liver failure in infants and young children and to identify clinical and biochemical markers for metabolic liver disease (MLD).

Methods: This study was conducted at Department of Pediatric Hepatology, in a tertiary care specialized centre for liver diseases. All children less than 3 y of age, with liver dysfunction and INR ≥2 were included in the study. They were managed as per the departmental protocol. Included children were divided based on the etiology into 2 groups: MLD and non MLD group. Comparison analysis (MLD vs. non MLD) of the clinical and biochemical parameters was done.

Results: There were 30 children under 3 y of age with acute liver failure (ALF) with median age of 12.5 mo. Fifteen children were less than 12 mo. MLD (33 %) and hemophagocytic lymphohistiocytosis (HLH) (17 %) together accounted for half of the cases of ALF in children below 3 y of age. The other common etiologies were drug induced liver injury and acute viral hepatitis A. Etiology remained indeterminate in 3 cases (10 %). Comparative analysis of the clinical and biochemical parameters between MLD and non MLD group showed significant difference between the two groups in the median values of age (p = 0.014), bilirubin (p = 0.017), jaundice to encephalopathy (JE) interval (p = 0.039) and blood sugar (p = 0.001). Suggestive family history (OR 3.73, 95 %CI 1.67-8.30), developmental delay (OR 4.4 95 %CI 2.03-9.51), presence of diarrhea/vomiting (OR 3.28, 95 %CI 1.32-8.13) in the history and presence of urinary non glucose reducing substance (NGRS) (OR 15.5, 95 %CI 2.26-106.87) were also significantly associated with MLD group. Only 40 % children survived with native liver.

Conclusions: MLD and HLH account for majority of ALF in infants. About 10 % of cases remain indeterminate. Viral hepatitis is more common in young children. Apart from clinical indicators, young age, high bilirubin, synthetic dysfunction, low sugar and NGRS in urine indicate MLD as a cause. Survival with native liver is low.

Keywords: Acute liver failure; Etiology; Hemophagocytosis; Infants; Markers; Metabolic liver diseases.

Publication types

Comparative Study

MeSH terms

Biomarkers / metabolism
Chemical and Drug Induced Liver Injury / complications
Child, Preschool
Female
Hepatitis A / complications
Humans
India
Infant
Liver / physiopathology
Liver Failure, Acute / etiology*
Liver Failure, Acute / metabolism
Liver Failure, Acute / physiopathology
Male
Tertiary Care Centers

Substances

Biomarkers