Congenital Heart Defect
Gene: FGD5
PMID 41574350 Steffes et al 2026 - identified a de novo NMD predicted FGD5 variant in a 30+3 week old infant with pulmonary artery stenosis and progressive pulmonary arterial hypertension.
PMID 32037394 Reuters et al 2020 - identified a maternally inherited, heterozygous, NMD-predicted variant (p.Glu322*) in a child with pulmonary stenosis, ASD and micrognathia.
PMID 30232381 Reuters et al 2019 - identified an NMD-predicted variant (p.Arg1225*) in an adult with congenital heart disease with no familial segregation information provided.
FGD5 implicated in VEGF pathway and expressed in endothelial cells. pLI score of 1.0. Highest het count in gnomAD for an NMD-predicted PTC variant is 9. Presence of multiple transcripts could contribute to variable expressivity and incomplete penetrance. However, given background prevalence of congenital heart disease, more case-level evidence is required to upgrade this gene-disease association to Green,
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Comment on other evidence:
PMID: 41199744 Liu et al 2025 report a heterozygous FGD5 missense variant c.3233C>A, p.T1078K in a fetus with pulmonary artery stenosis. Variant was inherited from an apparently unaffected mother of East Asian ancestry. Whilst this variant is absent from gnomAD v4 - this ancestral group is underrepresented and an alt change with a higher Grantham score at the same residue (Thr --> Ile) is present in 325 hets.
FDG5 knockout mouse demonstrated embryonic lethality, no haploinsufficiency animal model currently available.Created: 19 Feb 2026, 10:55 a.m. | Last Modified: 19 Feb 2026, 10:55 a.m.
Panel Version: 1.4336
Mode of inheritance
MONOALLELIC, autosomal or pseudoautosomal, NOT imprinted
Phenotypes
Congenital heart disease - MONDO:0005453, FGD5-related
Publications
Appears to be two separate families reported with different nonsense variants in FGD5 associated with TOF. There is some author and recruitment overlap however there is no compelling evidence to state the two probands are related.
32037394 - one family reported with a nonsense variant in an individual with pulmonary stenosis and dysplastic valve, ASD - Glu322* (variant is absent in gnomAD v4.1)
30232381 (missed this publication) - individual reported with TOF, ASD, AF, hypertension, aortic dilation Arg1225* - present in gnomADv4.1 singleton in EAS population.
There is no clear evidence that LoF is the mechanism of disease. No pathogenic variants have been reported in ClinVar at this stage thus the gene should remain as Red till further evidence is provided.
Sources: LiteratureCreated: 26 Nov 2025, 10:02 a.m.
Mode of inheritance
MONOALLELIC, autosomal or pseudoautosomal, NOT imprinted
Phenotypes
tetralogy of fallot MONDO:0008542
Publications
Phenotypes for gene: FGD5 were changed from Congenital heart disease - MONDO:0005453, FGD5-related to Congenital heart disease - MONDO:0005453, FGD5-related
Phenotypes for gene: FGD5 were changed from tetralogy of fallot MONDO:0008542 to Congenital heart disease - MONDO:0005453, FGD5-related
Publications for gene: FGD5 were set to 41574350; 41199744; 32037394; 30232381
Publications for gene: FGD5 were set to 32037394; 30232381
Gene: fgd5 has been classified as Amber List (Moderate Evidence).
Gene: fgd5 has been classified as Red List (Low Evidence).
gene: FGD5 was added gene: FGD5 was added to Congenital Heart Defect. Sources: Literature Mode of inheritance for gene: FGD5 was set to MONOALLELIC, autosomal or pseudoautosomal, NOT imprinted Publications for gene: FGD5 were set to 32037394; 30232381 Phenotypes for gene: FGD5 were set to tetralogy of fallot MONDO:0008542