Homozygous variant p. Arg90His in NCF1 is associated with early-onset Interferonopathy: a case report.
Oskar SchnappaufLiane HealeDilan DissanayakeWanxia L TsaiMassimo GadinaThomas L LetoDaniel L KastnerHarry L MalechDouglas B KuhnsIvona AksentijevichRonald M LaxerPublished in: Pediatric rheumatology online journal (2021)
Homozygosity for p.Arg90His in NCF1 should be considered contributory in young patients with an atypical systemic inflammatory antecedent phenotype that may evolve into autoimmunity later in life. The complex genomic organization of NCF1 poses a difficulty for high-throughput genotyping techniques and variants in this gene should be carefully evaluated when using the next generation and Sanger sequencing technologies. The p.Arg90His variant is found at a variable allele frequency in different populations, and is higher in people of South East Asian ancestry. In complex genetic diseases such as SLE, other rare and common susceptibility alleles might be necessary for the full disease expressivity.