A new multisystem ERCC1-hepatorenal syndrome: insights from a clinical cohort, molecular pathogenesis, and management guidelines

SM White; AP Wondergem; I Breet; M Dittmaier; K Bell; CM Richmond; W Hardikar; K Bhatia; C Quinlan; D Orchard; A D’Souza; WJ Chazin; C Smith; R Sparkes; S Lam; A Carter; RJ Hopkin; L Khendek; BR Sullivan; N Becher; AKW Simonsen; H Kvistgaard; K Dempsey; AG Miethke; PA Gregersen; E Phillips; MS Luijsterburg

Journal article

A new multisystem ERCC1-hepatorenal syndrome: insights from a clinical cohort, molecular pathogenesis, and management guidelines

SM White, AP Wondergem, I Breet, M Dittmaier, K Bell, CM Richmond, W Hardikar, K Bhatia, C Quinlan, D Orchard, A D’Souza, WJ Chazin, C Smith, R Sparkes, S Lam, A Carter, RJ Hopkin, L Khendek, BR Sullivan, N Becher Show all

European Journal of Human Genetics | Published : 2025

DOI: 10.1038/s41431-025-01910-0

Abstract

DNA repair disorders are a group of conditions characterized by progressive, multisystem phenotypes. Defining new clinical presentations of these disorders is essential for optimizing patient care. ERCC1-XPF is a multifunctional endonuclease involved in nucleotide excision repair (NER) and interstrand crosslink (ICL) repair. We sought to define a novel multisystem phenotype associated with biallelic ERCC1 variants and impaired DNA repair. Through international collaboration, we identified seven individuals from five families carrying biallelic ERCC1 variants, including p.Arg156Trp and p.Ala266Pro, who exhibited a distinct clinical phenotype. All individuals presented with growth restriction,..

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