NAA10 mutation causing a novel intellectual disability syndrome with Long QT due to N-terminal acetyltransferase impairment

Casey, Jillian P.; Støve, Svein Isungset; McGorrian, Catherine; Galvin, Joseph; Blenski, Marina; Dunne, Aimee; Ennis, Sean; Brett, Francesca; King, Mary D.; Arnesen, Thomas; Lynch, Sally Ann

doi:10.1038/srep16022

Cited by 73 publications

(109 citation statements)

References 35 publications

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“…NAA10 is associated with Ogden syndrome, an X‐linked neurodevelopment disorder (MIM#300013). Ogden syndrome can be caused by both X‐linked dominant inheritance with a milder phenotype, or X‐linked recessive inheritance with severe phenotypes, and the syndrome is characterized by postnatal growth failure, delayed psychomotor development, ID, hypotonia, and dysmorphic features (Casey et al, ; Popp et al, ; Rope et al, ). The phenotype thus shows some shared features with the phenotype reported for patients with NAA15 DNVs.…”

Section: Discussionmentioning

confidence: 99%

Exome sequencing reveals NAA15 and PUF60 as candidate genes associated with intellectual disability

Zhao

Halvardson

Zander

et al. 2017

American J of Med Genetics Pt B

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Intellectual Disability (ID) is a clinically heterogeneous condition that affects 2–3% of population worldwide. In recent years, exome sequencing has been a successful strategy for studies of genetic causes of ID, providing a growing list of both candidate and validated ID genes. In this study, exome sequencing was performed on 28 ID patients in 27 patient‐parent trios with the aim to identify de novo variants (DNVs) in known and novel ID associated genes. We report the identification of 25 DNVs out of which five were classified as pathogenic or likely pathogenic. Among these, a two base pair deletion was identified in the PUF60 gene, which is one of three genes in the critical region of the 8q24.3 microdeletion syndrome (Verheij syndrome). Our result adds to the growing evidence that PUF60 is responsible for the majority of the symptoms reported for carriers of a microdeletion across this region. We also report variants in several genes previously not associated with ID, including a de novo missense variant in NAA15. We highlight NAA15 as a novel candidate ID gene based on the vital role of NAA15 in the generation and differentiation of neurons in neonatal brain, the fact that the gene is highly intolerant to loss of function and coding variation, and previously reported DNVs in neurodevelopmental disorders.

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Section: Discussionmentioning

confidence: 99%

Exome sequencing reveals NAA15 and PUF60 as candidate genes associated with intellectual disability

Zhao

Halvardson

Zander

et al. 2017

American J of Med Genetics Pt B

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“…Y43S (exon 3), causing an intellectual disability syndrome with facial dysmorphic features, hypotonia, scoliosis and long QT due to NAT impairment [127]. Saunier and colleagues identified three novel Naa10 mutations; the R83C mutation was detected in a male and seven girls, while the F128L mutation and F128I was detected in a girl each [128].…”

Section: Accepted Manuscriptmentioning

confidence: 98%

The world of protein acetylation

Drazic

Myklebust

Ree

et al. 2016

Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics

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659

532

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Acetylation is one of the major post-translational protein modifications in the cell, with manifold effects on the protein level as well as on the metabolome level. The acetyl group, donated by the metabolite acetyl-coenzyme A, can be co- or post-translationally attached to either the α-amino group of the N-terminus of proteins or to the ε-amino group of lysine residues. These reactions are catalyzed by various N-terminal and lysine acetyltransferases. In case of lysine acetylation, the reaction is enzymatically reversible via tightly regulated and metabolism-dependent mechanisms. The interplay between acetylation and deacetylation is crucial for many important cellular processes. In recent years, our understanding of protein acetylation has increased significantly by global proteomics analyses and in depth functional studies. This review gives a general overview of protein acetylation and the respective acetyltransferases, and focuses on the regulation of metabolic processes and physiological consequences that come along with protein acetylation.

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“…Since the first description of Ogden syndrome in two multiplex unrelated families, additional variants in Naa10 have been identified in other probands with non‐syndromic intellectual disabilities accompanied by postnatal growth failure and skeletal anomalies (Rauch et al, ; Popp et al, ; Saunier et al, ), one family with two brothers with syndromic intellectual disability with long QT, a prologation of the depolarization and repolarization interval of the ventricles of the heart (Casey et al, ) and one multiplex family with Lenz microphthalmia syndrome, characterized by microphthalmia or anophthalmia, developmental delay, intellectual disability, skeletal abnormalities and malformations of teeth, fingers and toes (Esmailpour et al, ). The phenotypic differences between all cases are fairly distinct, and to date there has been no unifying explanation for this, beyond just genetic background differences.…”

Section: Introductionmentioning

confidence: 99%

Proteomic and genomic characterization of a yeast model for Ogden syndrome

Dörfel

Han

Crain

et al. 2016

Yeast

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Naa10 is an Nα‐terminal acetyltransferase that, in a complex with its auxiliary subunit Naa15, co‐translationally acetylates the α‐amino group of newly synthetized proteins as they emerge from the ribosome. Roughly 40–50% of the human proteome is acetylated by Naa10, rendering this an enzyme one of the most broad substrate ranges known. Recently, we reported an X‐linked disorder of infancy, Ogden syndrome, in two families harbouring a c.109 T > C (p.Ser37Pro) variant in NAA10. In the present study we performed in‐depth characterization of a yeast model of Ogden syndrome. Stress tests and proteomic analyses suggest that the S37P mutation disrupts Naa10 function and reduces cellular fitness during heat shock, possibly owing to dysregulation of chaperone expression and accumulation. Microarray and RNA‐seq revealed a pseudo‐diploid gene expression profile in ΔNaa10 cells, probably responsible for a mating defect. In conclusion, the data presented here further support the disruptive nature of the S37P/Ogden mutation and identify affected cellular processes potentially contributing to the severe phenotype seen in Ogden syndrome. Data are available via GEO under identifier GSE86482 or with ProteomeXchange under identifier PXD004923. © 2016 The Authors. Yeast published by John Wiley & Sons, Ltd.

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NAA10 mutation causing a novel intellectual disability syndrome with Long QT due to N-terminal acetyltransferase impairment

Cited by 73 publications

References 35 publications

Exome sequencing reveals NAA15 and PUF60 as candidate genes associated with intellectual disability

Exome sequencing reveals NAA15 and PUF60 as candidate genes associated with intellectual disability

The world of protein acetylation

Proteomic and genomic characterization of a yeast model for Ogden syndrome

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