METAP1 mutation is a novel candidate for autosomal recessive intellectual disability.
Ahmet Okay CaglayanFesih AktarKaya BilguvarJacob F BaranoskiGozde Tugce AkgumusAkdes Serin HarmanciEmine Zeynep Erson-OmayKatsuhito YasunoHuseyin CaksenMurat GunelPublished in: Journal of human genetics (2020)
Intellectual disability (ID) is a genetic and clinically heterogeneous common disease and underlying molecular pathogenesis can frequently not be identified by whole-exome/genome testing. Here, we report four siblings born to a consanguineous union who presented with intellectual disability and discuss the METAP1 pathway as a novel etiology of ID. Genomic analyses demonstrated that patients harbor a novel homozygous nonsense mutation in the gene METAP1. METAP1 codes for methionine aminopeptidase 1 (MetAP1) which oversees the co-translational excision of the first methionine remnants in eukaryotes. The loss-of-function mutations to this gene may result in a defect in the translation of many essential proteins within a cell. Improper neuronal function resulting from this loss of essential proteins could lead to neurologic impairment and ID.
Keyphrases
- intellectual disability
- copy number
- autism spectrum disorder
- genome wide
- end stage renal disease
- ejection fraction
- newly diagnosed
- chronic kidney disease
- prognostic factors
- dna methylation
- single cell
- patient reported outcomes
- peritoneal dialysis
- cell therapy
- amino acid
- gene expression
- genome wide identification
- single molecule
- blood brain barrier
- transcription factor
- preterm infants