6533b85bfe1ef96bd12bb6a6

RESEARCH PRODUCT

Expanding the Phenotype Associated with NAA10-Related N-Terminal Acetylation Deficiency

Alice MasurelYannis DuffourdBénédicte GérardChristiane ZweierThomas ArnesenThomas ArnesenBernt PoppMelissa P. WassersteinCyril MignotNicholas AhmewLaetitia LampertBoris KerenJean Baptiste RivièreCaroline NavaLaurence FaivreChloé SaunierMarjon Van SlegtenhorstPaul KuentzChristel Thauvin-robinetMarina BlenskiSvein Isungset StøveSvein Isungset StøvePaula GoldenbergAmélie PitonAndré ReisJulien ThevenonFrédéric HuetAnge Line BruelGrazia M.s. ManciniKamer TezcanCharlotte De BieBruno LeheupBertrand Isidor

subject

0301 basic medicineMaleModels MolecularMicrocephalyMutation MissenseBiologyGermlineKEY WORDS: NAA1003 medical and health sciencesGermline mutationGenes X-LinkedIntellectual disabilityGeneticsmedicineMissense mutationHumansGenetic Predisposition to DiseaseN-Terminal Acetyltransferase EGenetics (clinical)Genetic Association StudiesGerm-Line MutationN-Terminal Acetyltransferase AResearch ArticlesGeneticsX-linked[SDV.GEN]Life Sciences [q-bio]/GeneticsRegional Council of BurgundyMosaicismN-terminal acetylationAcetylationmedicine.diseasePhenotypePedigreeOgden SyndromeX‐linked030104 developmental biologyNAA10intellectual disabilityN‐terminal acetylationContract grant sponsors: Dijon University HospitalFemale[ SDV.GEN ] Life Sciences [q-bio]/GeneticsNAA15Research Article

description

International audience; N-terminal acetylation is a common protein modification in eukaryotes associated with numerous cellular processes. Inherited mutations in NAA10, encoding the catalytic subunit of the major N-terminal acetylation complex NatA have been associated with diverse, syndromic X-linked recessive disorders, whereas de novo missense mutations have been reported in one male and one female individual with severe intellectual disability but otherwise unspecific phenotypes. Thus, the full genetic and clinical spectrum of NAA10 deficiency is yet to be delineated. We identified three different novel and one known missense mutation in NAA10, de novo in 11 females, and due to maternal germ line mosaicism in another girl and her more severely affected and deceased brother. In vitro enzymatic assays for the novel, recurrent mutations p.(Arg83Cys) and p.(Phe128Leu) revealed reduced catalytic activity. X-inactivation was random in five females. The core phenotype of X-linked NAA10-related N-terminal-acetyltransferase deficiency in both males and females includes developmental delay, severe intellectual disability, postnatal growth failure with severe microcephaly, and skeletal or cardiac anomalies. Genotype–phenotype correlations within and between both genders are complex and may include various factors such as location and nature of mutations, enzymatic stability and activity, and X-inactivation in females.

yearjournalcountryeditionlanguage
2016-04-01Human Mutation
10.1002/humu.23001https://doi.org/10.1002/humu.23001