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Naturally occurring splice variants dissect the functional domains of BHC80 and emphasize the need for RNA analysis.

Duha HejlaStephanie HuynhSimran SamraPhillip A RichmondJoshua DalmannKate L Del BelLoryn ByresAnna LehmanStuart E TurveyElizabeth M J Lee
Published in: American journal of medical genetics. Part A (2024)
Pathogenic PHF21A variation causes PHF21A-related neurodevelopmental disorders (NDDs). Although amorphic alleles, including haploinsufficiency, have been established as a disease mechanism, increasing evidence suggests that missense variants as well as frameshift variants extending the BHC80 carboxyl terminus also cause disease. Expanding on these, we report a proposita with intellectual disability and overgrowth and a novel de novo heterozygous PHF21A splice variant (NM_001352027.3:c.[153+1G>C];[=]) causing skipping of exon 6, which encodes an in-frame BHC80 deletion (p.(Asn30_Gln51del)). This deletion disrupts a predicted leucine zipper domain and implicates this domain in BHC80 function and as a target of variation causing PHF21A-related NDDs. This extension of understanding emphasizes the application of RNA analysis in precision genomic medicine practice.
Keyphrases
  • intellectual disability
  • copy number
  • autism spectrum disorder
  • healthcare
  • primary care
  • photodynamic therapy
  • gene expression
  • genome wide
  • nucleic acid
  • congenital heart disease