Whole-exome Sequencing for Genetic Diagnosis of Idiopathic Liver Injury in Children

Overview

Journal J Cell Mol Med

Specialties Cell Biology
Molecular Biology

Date 2024 Jun 12

PMID 38864694

Authors

Aysima Atilgan Lulecioglu

Yilmaz Yucehan Yazici

Alperen Baran

Khaled Warasnhe

Sengul Beyaz

Caner Aytekin

Figen Ozcay

Yusuf Aydemir

Zeren Baris

Serkan Belkaya

Affiliations

Soon will be listed here.

Abstract

Genome-wide approaches, such as whole-exome sequencing (WES), are widely used to decipher the genetic mechanisms underlying inter-individual variability in disease susceptibility. We aimed to dissect inborn monogenic determinants of idiopathic liver injury in otherwise healthy children. We thus performed WES for 20 patients presented with paediatric-onset recurrent elevated transaminases (rELT) or acute liver failure (ALF) of unknown aetiology. A stringent variant screening was undertaken on a manually-curated panel of 380 genes predisposing to inherited human diseases with hepatobiliary involvement in the OMIM database. We identified rare nonsynonymous variants in nine genes in six patients (five rELT and one ALF). We next performed a case-level evaluation to assess the causal concordance between the gene mutated and clinical symptoms of the affected patient. A genetic diagnosis was confirmed in four rELT patients (40%), among whom two carried novel mutations in ACOX2 or PYGL, and two had previously-reported morbid variants in ABCB4 or PHKA2. We also detected rare variants with uncertain clinical significance in CDAN1, JAG1, PCK2, SLC27A5 or VPS33B in rELT or ALF patients. In conclusion, implementation of WES improves diagnostic yield and enables precision management in paediatric cases of liver injury with unknown aetiology, in particular recurrent hypertransaminasemia.

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