The p.Thr395Met missense variant of NFIA found in a patient with intellectual disability is a defective variant.
Yurie OguraTomoko UeharaKota UjibeHiroshi YoshihashiMamiko YamadaHisato SuzukiToshiki TakenouchiKenjiro KosakiHiromi HirataPublished in: American journal of medical genetics. Part A (2022)
Nuclear factor one A (NFIA) is a transcription factor that regulates the development of the central nervous system. Haploinsufficiency of the NFIA gene causes NFIA-related disorder, which includes brain abnormalities and intellectual disability, with or without urinary tract defects. Intragenic deletions, nonsense variants, frameshift variants, and missense variants in one allele of the NFIA gene have been reported to cause various neurological and urogenital symptoms. Here we report a 10-year-old male patient with developmental delay, coarctation of the aorta, and distinctive facial features. Exome analysis identified a rare de novo heterozygous missense variant p.Thr395Met in NFIA. We employed zebrafish as a model organism in our NFIA analysis and found that nfia -/- zebrafish initially showed a loss of commissural axons in the brain, and eventually underwent growth retardation resulting in premature death. Impairment of the commissural neurons in nfia -/- zebrafish embryos could be restored by the expression of wild-type human NFIA protein, but not of mutant human protein harboring the p.Thr395Met substitution, indicating that this variant affects the function of NFIA protein. Taken together, we suggest that the p.Thr395Met allele in the NFIA gene is relevant to the pathogenesis of NFIA-related disorder.
Keyphrases
- intellectual disability
- copy number
- autism spectrum disorder
- endothelial cells
- transcription factor
- nuclear factor
- wild type
- tyrosine kinase
- binding protein
- toll like receptor
- protein protein
- genome wide identification
- amino acid
- case report
- early onset
- blood brain barrier
- resting state
- poor prognosis
- depressive symptoms
- multiple sclerosis
- coronary artery
- brain injury
- pulmonary hypertension
- urinary tract
- pulmonary artery
- cerebrospinal fluid
- aortic valve
- sleep quality