Higher Promoter Methylation of the Ubiquitin-Associated and SH3 Domain Containing A (UBASH3A) Gene Is Associated With T-Lymphocyte Ontogeny and Reduced Susceptibility to Early-Onset Sepsis

We investigated the genetic and epigenetic regulation of the UBASH3A gene and its association with early-onset sepsis. Using matched whole blood DNA methylation, gene expression, genotypes, and immune cell counts from the EPIC-HIPC newborn cohort, we report that promoter methylation was negatively correlated with ontogenetic changes in UBASH3A gene expression and circulating CD3+ T-cell numbers.

Citation:
Wang Z, Amenyogbe N, Ben-Othman R, Cai B, Lo M, ……. Richmond P, Tebbutt SJ, ………. Kollmann TR, Martino D. Higher Promoter Methylation of the Ubiquitin-Associated and SH3 Domain Containing A (UBASH3A) Gene Is Associated With T-Lymphocyte Ontogeny and Reduced Susceptibility to Early-Onset Sepsis. J Infect Dis. 2026;233(3):e706-e11.

Keywords:
DNA methylation; UBASH3A; neonatal sepsis; ontogeny

Abstract:
We investigated the genetic and epigenetic regulation of the UBASH3A gene and its association with early-onset sepsis. Using matched whole blood DNA methylation, gene expression, genotypes, and immune cell counts from the EPIC-HIPC newborn cohort, we report that promoter methylation was negatively correlated with ontogenetic changes in UBASH3A gene expression and circulating CD3+ T-cell numbers.

Our investigators

Peter Richmond

MBBS MRCP(UK) FRACP

Head, Vaccine Trials Group

Professor Tobias Kollmann

PhD, M.D., SFUW

Honorary Research Associate

Tobias.Kollmann@thekids.org.au

08 6319 1050

David Martino

BSc PhD

Head, Chronic Diseases Research

David.Martino@thekids.org.au