# A novel splicing variant in NBAS identified by minigene assay causes infantile liver failure syndrome type 2

**Authors:** Anna Hu, Jun Liang, Hongbo Liu, Jinghui Jiang, Fujing Xie, Xin Zhou, Xiaojia Zhang

PMC · DOI: 10.3389/fgene.2025.1687266 · Frontiers in Genetics · 2025-10-08

## TL;DR

A new splicing variant in the NBAS gene causes infantile liver failure syndrome type 2, confirmed through genetic and functional testing.

## Contribution

A novel splice-site variant in NBAS is identified as pathogenic through minigene splicing assays and genomic analysis.

## Key findings

- The c.1600-1G>T variant in NBAS causes aberrant splicing and abnormal transcripts.
- Compound heterozygous NBAS variants were found in a patient with ILFS2.
- Functional validation confirms the pathogenicity of the novel splicing variant.

## Abstract

Infantile liver failure syndrome type 2 (ILFS2) is an autosomal recessive disorder caused by biallelic NBAS variants, characterized by recurrent acute liver failure (ALF) typically triggered by febrile episodes.

Trio-based whole-exome sequencing (Trio-WES) was performed on a child with recurrent ALF and both parents. Candidate variants were validated in family members by Sanger sequencing, and the functional impact of a novel splice-site variant was assessed using a minigene splicing assay.

Trio-WES revealed compound heterozygous NBAS variants in the proband: the known pathogenic variant c.3596G>A (p.Cys1199Tyr) and a novel splice-site variant c.1600-1G>T. The c.1600-1G>T variant was classified as pathogenic based on ACMG criteria, supported by SpliceAI analysis predicting potential splicing abnormalities with the following scores: acceptor gain (AG = 0.33 at −9 bp), acceptor loss (AL = 0.93 at −1 bp), donor gain (DG = 0.00 at −8 bp), and donor loss (DL = 0.25 at −126 bp). Minigene assays confirmed that c.1600-1G>T causes aberrant pre-mRNA splicing, resulting in multiple abnormal transcripts—including 185 bp and 56 bp intron 15 retention, an 8 bp deletion within exon 16, and full exon 16 skipping—predicted to produce truncated or internally deleted NBAS proteins, providing functional evidence of pathogenicity.

We report a novel pathogenic splicing variant in NBAS that causes ILFS2 in compound heterozygosity. This finding underscores the importance of integrating genomic sequencing with functional validation for accurate diagnosis and genetic counseling.

## Linked entities

- **Genes:** NBAS (NBAS subunit of NRZ tethering complex) [NCBI Gene 51594]
- **Diseases:** infantile liver failure syndrome type 2 (MONDO:0014659), acute liver failure (MONDO:0019542)

## Full-text entities

- **Genes:** NBAS (NBAS subunit of NRZ tethering complex) [NCBI Gene 51594] {aka ILFS2, NAG, SOPH}
- **Diseases:** ILFS2 (OMIM:616483), ALF (MESH:D017114), autosomal recessive disorder (MESH:D030342)
- **Mutations:** c.1600-1G>T, c.3596G>A, p.Cys1199Tyr

## Full text

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## Figures

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## References

21 references — full list in the complete paper: https://tomesphere.com/paper/PMC12542828/full.md

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Source: https://tomesphere.com/paper/PMC12542828