NAA10 polyadenylation signal variants cause syndromic microphthalmia.
Jennifer J JohnstonKathleen A WilliamsonChristopher M ChouJulie C SappMorad AnsariHeather M ChapmanDavid N CooperTabib DabirJeffrey N DudleyRichard J HoltNicola K RaggeAlejandro A SchäfferShurjo K SenAnne M SlavotinekDavid R FitzPatrickThomas M GlaserFiona StewartGraeme Cm BlackLeslie G BieseckerPublished in: Journal of medical genetics (2019)
These data show that PAS variants are the most common variant type in NAA10-associated syndromic microphthalmia, suggesting reduced RNA is the molecular mechanism by which these alterations cause microphthalmia/anophthalmia. We reviewed recognised variants in PAS associated with Mendelian disorders and identified only 23 others, indicating that NAA10 harbours more than 10% of all known PAS variants. We hypothesise that PAS in other genes harbour unrecognised pathogenic variants associated with Mendelian disorders. The systematic interrogation of PAS could improve genetic testing yields.