ClinGen Dosage Sensitivity Curation Page

HDAC8

  • Curation Status: Complete

Location Information

Select assembly: (NC_000023.10) (NC_000023.11)
Evidence for haploinsufficiency phenotype
PubMed ID Description
22885700 Deardorff MA et al identified four de novo missense mutations and one de novo nonsense HDAC8 mutations in 6 CdLS probands. None of the mutations was seen in 290 ethnically matched control chromosomes or in 629 individuals of the 1000 Genomes Project. All probands were diagnosed of CdLS, pre-screened and were negative for mutations in NIPBL, SMC1A and SMC3.
24403048 Kaiser FJ et al reported a cohort of 38 individuals with an emerging spectrum of features caused by HDAC8 mutations. The mutations were detected by whole-genome SNP array, and most are missense and de novo. To evaluate the effect of these mutations on protein function, they mapped mutations on crystal structure of HDAC8 and expressed each of the mutated protein in E. coli. The results showed varying loss of activity of HDAC8 protein.
26671848 Parenti I et al reported on the clinical and molecular characterization of 11 patients carrying 10 distinct variants in HDAC8. They used different approaches including Sanger sequencing, a targetd NGS panel including the five known CdLS genes, and whole exome sequencing. The variants include one exchange affecting a conserved splice donor site (c.910+1G>A), one nonsense variant p.(R166*), one frame-shift deletion p.(F207Nfs*3) and seven single amino acid substitutions, namely p.(S150P), p.(C153R), p.(N156K), p.(T280I), p.(P257L), p.(C287Y), and p.(G320R).

The loss-of-function and triplosensitivity ratings for genes on the X chromosome are made in the context of a male genome to account for the effects of hemizygous duplications or nullizygous deletions. In contrast, disruption of some genes on the X chromosome causes male lethality and the ratings of dosage sensitivity instead take into account the phenotype in female individuals. Factors that may affect the severity of phenotypes associated with X-linked disorders include the presence of variable copies of the X chromosome (i.e. 47,XXY or 45,X) and skewed X-inactivation in females.

  • Triplosensitivity score: 0
  • Strength of Evidence (disclaimer): No evidence for dosage pathogenicity

The loss-of-function and triplosensitivity ratings for genes on the X chromosome are made in the context of a male genome to account for the effects of hemizygous duplications or nullizygous deletions. In contrast, disruption of some genes on the X chromosome causes male lethality and the ratings of dosage sensitivity instead take into account the phenotype in female individuals. Factors that may affect the severity of phenotypes associated with X-linked disorders include the presence of variable copies of the X chromosome (i.e. 47,XXY or 45,X) and skewed X-inactivation in females.