Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly

PURPOSE: N-terminal acetyltransferases modify proteins by adding an acetyl moiety to the first amino acid and are vital for protein and cell function. The NatB complex acetylates 20% of the human proteome and is composed of the catalytic subunit NAA20 and the auxiliary subunit NAA25. In five individ...

Descripción completa

Detalles Bibliográficos
Autores principales: Morrison, Jennifer, Altuwaijri, Norah K., Brønstad, Kirsten, Aksnes, Henriette, Alsaif, Hessa S., Evans, Anthony, Hashem, Mais, Wheeler, Patricia G., Webb, Bryn D., Alkuraya, Fowzan S., Arnesen, Thomas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group US 2021
Materias:
Brief Communication
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8553619/
https://www.ncbi.nlm.nih.gov/pubmed/34230638
http://dx.doi.org/10.1038/s41436-021-01264-0
_version_ 1784591618499674112
author Morrison, Jennifer
Altuwaijri, Norah K.
Brønstad, Kirsten
Aksnes, Henriette
Alsaif, Hessa S.
Evans, Anthony
Hashem, Mais
Wheeler, Patricia G.
Webb, Bryn D.
Alkuraya, Fowzan S.
Arnesen, Thomas
author_facet Morrison, Jennifer
Altuwaijri, Norah K.
Brønstad, Kirsten
Aksnes, Henriette
Alsaif, Hessa S.
Evans, Anthony
Hashem, Mais
Wheeler, Patricia G.
Webb, Bryn D.
Alkuraya, Fowzan S.
Arnesen, Thomas
author_sort Morrison, Jennifer
collection PubMed
description PURPOSE: N-terminal acetyltransferases modify proteins by adding an acetyl moiety to the first amino acid and are vital for protein and cell function. The NatB complex acetylates 20% of the human proteome and is composed of the catalytic subunit NAA20 and the auxiliary subunit NAA25. In five individuals with overlapping phenotypes, we identified recessive homozygous missense variants in NAA20. METHODS: Two different NAA20 variants were identified in affected individuals in two consanguineous families by exome and genome sequencing. Biochemical studies were employed to assess the impact of the NAA20 variants on NatB complex formation and catalytic activity. RESULTS: Two homozygous variants, NAA20 p.Met54Val and p.Ala80Val (GenBank: NM_016100.4, c.160A>G and c.239C>T), segregated with affected individuals in two unrelated families presenting with developmental delay, intellectual disability, and microcephaly. Both NAA20-M54V and NAA20-A80V were impaired in their capacity to form a NatB complex with NAA25, and in vitro acetylation assays revealed reduced catalytic activities toward different NatB substrates. Thus, both NAA20 variants are impaired in their ability to perform cellular NatB-mediated N-terminal acetylation. CONCLUSION: We present here a report of pathogenic NAA20 variants causing human disease and data supporting an essential role for NatB-mediated N-terminal acetylation in human development and physiology. GRAPHICAL ABSTRACT: [Image: see text]
format Online
Article
Text
id pubmed-8553619
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Nature Publishing Group US
record_format MEDLINE/PubMed
spelling pubmed-85536192021-11-04 Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly Morrison, Jennifer Altuwaijri, Norah K. Brønstad, Kirsten Aksnes, Henriette Alsaif, Hessa S. Evans, Anthony Hashem, Mais Wheeler, Patricia G. Webb, Bryn D. Alkuraya, Fowzan S. Arnesen, Thomas Genet Med Brief Communication PURPOSE: N-terminal acetyltransferases modify proteins by adding an acetyl moiety to the first amino acid and are vital for protein and cell function. The NatB complex acetylates 20% of the human proteome and is composed of the catalytic subunit NAA20 and the auxiliary subunit NAA25. In five individuals with overlapping phenotypes, we identified recessive homozygous missense variants in NAA20. METHODS: Two different NAA20 variants were identified in affected individuals in two consanguineous families by exome and genome sequencing. Biochemical studies were employed to assess the impact of the NAA20 variants on NatB complex formation and catalytic activity. RESULTS: Two homozygous variants, NAA20 p.Met54Val and p.Ala80Val (GenBank: NM_016100.4, c.160A>G and c.239C>T), segregated with affected individuals in two unrelated families presenting with developmental delay, intellectual disability, and microcephaly. Both NAA20-M54V and NAA20-A80V were impaired in their capacity to form a NatB complex with NAA25, and in vitro acetylation assays revealed reduced catalytic activities toward different NatB substrates. Thus, both NAA20 variants are impaired in their ability to perform cellular NatB-mediated N-terminal acetylation. CONCLUSION: We present here a report of pathogenic NAA20 variants causing human disease and data supporting an essential role for NatB-mediated N-terminal acetylation in human development and physiology. GRAPHICAL ABSTRACT: [Image: see text] Nature Publishing Group US 2021-07-06 2021 /pmc/articles/PMC8553619/ /pubmed/34230638 http://dx.doi.org/10.1038/s41436-021-01264-0 Text en © The Author(s) 2021 https://creativecommons.org/licenses/by/4.0/Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Brief Communication
Morrison, Jennifer
Altuwaijri, Norah K.
Brønstad, Kirsten
Aksnes, Henriette
Alsaif, Hessa S.
Evans, Anthony
Hashem, Mais
Wheeler, Patricia G.
Webb, Bryn D.
Alkuraya, Fowzan S.
Arnesen, Thomas
Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly
title Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly
title_full Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly
title_fullStr Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly
title_full_unstemmed Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly
title_short Missense NAA20 variants impairing the NatB protein N-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly
title_sort missense naa20 variants impairing the natb protein n-terminal acetyltransferase cause autosomal recessive developmental delay, intellectual disability, and microcephaly
topic Brief Communication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8553619/
https://www.ncbi.nlm.nih.gov/pubmed/34230638
http://dx.doi.org/10.1038/s41436-021-01264-0
work_keys_str_mv AT morrisonjennifer missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT altuwaijrinorahk missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT brønstadkirsten missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT aksneshenriette missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT alsaifhessas missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT evansanthony missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT hashemmais missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT wheelerpatriciag missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT webbbrynd missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT alkurayafowzans missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly
AT arnesenthomas missensenaa20variantsimpairingthenatbproteinnterminalacetyltransferasecauseautosomalrecessivedevelopmentaldelayintellectualdisabilityandmicrocephaly

Ejemplares similares