Frontiers in Pediatrics (May 2021)

Hepatic Presentation of Late-Onset Multiple Acyl-CoA Dehydrogenase Deficiency (MADD): Case Report and Systematic Review

  • Maria Anna Siano,
  • Claudia Mandato,
  • Lucia Nazzaro,
  • Gennaro Iannicelli,
  • Gian Paolo Ciccarelli,
  • Ferdinando Barretta,
  • Ferdinando Barretta,
  • Cristina Mazzaccara,
  • Cristina Mazzaccara,
  • Margherita Ruoppolo,
  • Margherita Ruoppolo,
  • Giulia Frisso,
  • Giulia Frisso,
  • Carlo Baldi,
  • Salvatore Tartaglione,
  • Francesco Di Salle,
  • Daniela Melis,
  • Daniela Melis,
  • Pietro Vajro,
  • Pietro Vajro,
  • Pietro Vajro

DOI
https://doi.org/10.3389/fped.2021.672004
Journal volume & issue
Vol. 9

Abstract

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Diagnosis of pediatric steatohepatitis is a challenging issue due to a vast number of established and novel causes. Here, we report a child with Multiple Acyl-CoA Dehydrogenase Deficiency (MADD) presenting with an underrated muscle weakness, exercise intolerance and an atypically severe steatotic liver involvement. A systematic literature review of liver involvement in MADD was performed as well. Our patient is a 11-year-old otherwise healthy, non-obese, male child admitted for some weakness/asthenia, vomiting and recurrent severe hypertransaminasemia (aspartate and alanine aminotransferases up to ×20 times upper limit of normal). Hepatic ultrasound showed a bright liver. MRI detected mild lipid storage of thighs muscles. A liver biopsy showed a micro-macrovacuolar steatohepatitis with minimal fibrosis. Main causes of hypertransaminasemia were ruled out. Serum aminoacids (increased proline), acylcarnitines (increased C4-C18) and a large excretion of urinary glutaric acid, ethylmalonic, butyric, isobutyric, 2-methyl-butyric and isovaleric acids suggested a diagnosis of MADD. Serum acylcarnitines and urinary organic acids fluctuated overtime paralleling serum transaminases during periods of illness/catabolic stress, confirming their recurrent nature. Genetic testing confirmed the diagnosis [homozygous c.1658A > G (p.Tyr553Cys) in exon 12 of the ETFDH gene]. Lipid-restricted diet and riboflavin treatment rapidly ameliorated symptoms, hepatic ultrasonography/enzymes, and metabolic profiles. Literature review (37 retrieved eligible studies, 283 patients) showed that liver is an extramuscular organ rarely involved in late-onset MADD (70 patients), and that amongst 45 patients who had fatty liver only nine had severe presentation.Conclusion: MADD is a disorder with a clinically heterogeneous phenotype. Our study suggests that MADD warrants consideration in the work-up of obesity-unrelated severe steatohepatitis.

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