Distinct diagnostic trajectories in NBAS‐associated acute liver failure highlights the need for timely functional studies

Lauren S. Akesson; Rocio Rius; Natasha J. Brown; Jeremy Rosenbaum; Sarah Donoghue; Michael Stormon; Charmaine Chai; Esmeralda Bordador; Yiran Guo; Hakon Hakonarson; Alison G. Compton; David R. Thorburn; Sumudu Amarasekera; Justine Marum; Alisha Monaco; Crystle Lee; Belinda Chong; Sebastian Lunke; Zornitza Stark; John Christodoulou

doi:10.1002/jmd2.12280

JIMD Reports (May 2022)

Distinct diagnostic trajectories in NBAS‐associated acute liver failure highlights the need for timely functional studies

Lauren S. Akesson,
Rocio Rius,
Natasha J. Brown,
Jeremy Rosenbaum,
Sarah Donoghue,
Michael Stormon,
Charmaine Chai,
Esmeralda Bordador,
Yiran Guo,
Hakon Hakonarson,
Alison G. Compton,
David R. Thorburn,
Sumudu Amarasekera,
Justine Marum,
Alisha Monaco,
Crystle Lee,
Belinda Chong,
Sebastian Lunke,
Zornitza Stark,
John Christodoulou

Affiliations

Lauren S. Akesson: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Rocio Rius: Department of Paediatrics University of Melbourne Melbourne Victoria Australia
Natasha J. Brown: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Jeremy Rosenbaum: Department of Gastroenterology Royal Children's Hospital Melbourne Victoria Australia
Sarah Donoghue: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Michael Stormon: Department of Gastroenterology Children's Hospital Westmead Sydney New South Wales Australia
Charmaine Chai: Department of Gastroenterology Children's Hospital Westmead Sydney New South Wales Australia
Esmeralda Bordador: Department of Metabolic Medicine Royal Children's Hospital Melbourne Victoria Australia
Yiran Guo: Center for Applied Genomics Children's Hospital of Philadelphia Philadelphia Pennsylvania USA
Hakon Hakonarson: Center for Applied Genomics Children's Hospital of Philadelphia Philadelphia Pennsylvania USA
Alison G. Compton: Department of Paediatrics University of Melbourne Melbourne Victoria Australia
David R. Thorburn: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Sumudu Amarasekera: Department of Paediatrics University of Melbourne Melbourne Victoria Australia
Justine Marum: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Alisha Monaco: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Crystle Lee: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Belinda Chong: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Sebastian Lunke: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
Zornitza Stark: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia
John Christodoulou: Victorian Clinical Genetics Services, Murdoch Children's Research Institute Royal Children's Hospital Melbourne Victoria Australia

DOI: https://doi.org/10.1002/jmd2.12280
Journal volume & issue: Vol. 63, no. 3
pp. 240 – 249

Abstract

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Abstract Variants of uncertain significance (VUS) are commonly found following genomic sequencing, particularly in ethnically diverse populations that are underrepresented in large population databases. Functional characterization of VUS may assist in variant reclassification, however these studies are not readily available and often rely on research funding and good will. We present four individuals from three families at different stages of their diagnostic trajectory with recurrent acute liver failure (RALF) and biallelic NBAS variants, confirmed by either trio analysis or cDNA studies. Functional characterization was undertaken, measuring NBAS and p31 levels by Western blotting, demonstrating reduced NBAS levels in two of three families, and reduced p31 levels in all three families. These results provided functional characterization of the molecular impact of a missense VUS, allowing reclassification of the variant and molecular confirmation of NBAS‐associated RALF. Importantly, p31 was decreased in all individuals, including an individual with two missense variants where NBAS protein levels were preserved. These results highlight the importance of access to timely functional studies after identification of putative variants, and the importance of considering a range of assays to validate variants whose pathogenicity is uncertain. We suggest that funding models for genomic sequencing should consider incorporating capabilities for adjunct RNA, protein, biochemical, and other specialized tests to increase the diagnostic yield which will lead to improved medical care, increased equity, and access to molecular diagnoses for all patients.

Published in JIMD Reports

ISSN: 2192-8304 (Print); 2192-8312 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the endocrine glands. Clinical endocrinology; Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/21928312

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