| Literature DB >> 30825388 |
Diana Carli1, Elisa Giorgio2, Francesca Pantaleoni3, Alessandro Bruselles4, Sabina Barresi3, Evelise Riberi1, Francesco Licciardi1, Andrea Gazzin1, Giuseppina Baldassarre1, Simone Pizzi3, Marcello Niceta3, Francesca C Radio3, Cristina Molinatto1, Davide Montin1, Pier L Calvo5, Andrea Ciolfi3, Nicole Fleischer6, Giovanni B Ferrero1, Alfredo Brusco2,7, Marco Tartaglia3.
Abstract
The pathogenic variants in the neuroblastoma-amplified sequence (NBAS) are associated with a clinical spectrum involving the hepatic, skeletal, ocular, and immune systems. Here, we report on two unrelated subjects with a complex phenotype solved by whole-exome sequencing, who shared a synonymous change in NBAS that was documented to affect the transcript processing and co-occurring with a truncating change. Starting from these two cases, we systematically assessed the clinical information available for all subjects with biallelic NBAS pathogenic variants (73 cases in total). We revealed a recognizable facial profile (hypotelorism, thin lips, pointed chin, and "progeroid" appearance) determined by using DeepGestalt facial recognition technology, and we provide evidence for the occurrence of genotype-phenotype correlations. Notably, severe hepatic involvement was associated with variants affecting the NBAS-Nter and Sec39 domains, whereas milder liver involvement and immunodeficiency were generally associated with variants located at the N-terminus and C-terminus of the protein. Remarkably, no patient was reported to carry two nonsense variants, suggesting lethality of complete NBAS loss-of-function.Entities:
Keywords: NBAS; acute liver failure; face2gene; facial recognition technology; genotype-phenotype correlation; splicing variant
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Year: 2019 PMID: 30825388 DOI: 10.1002/humu.23734
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878