The ClinGen Evidence Repository is an FDA-recognized human genetic variant database containing expert-curated assertions regarding variants' pathogenicity and supporting evidence summaries. [Disclaimer]
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Variant: NM_000552.5(VWF):c.2561G>A (p.Arg854Gln)

CA114139

296 (ClinVar)

Gene: VWF
Condition: von Willebrand disease type 2N
Inheritance Mode: Autosomal recessive inheritance
UUID: 01c59bbd-0d03-488a-94f1-fa68f3b2e083
Approved on: 2024-07-09
Published on: 2024-08-12

HGVS expressions

NM_000552.5:c.2561G>A
NM_000552.5(VWF):c.2561G>A (p.Arg854Gln)
NC_000012.12:g.6034812C>T
CM000674.2:g.6034812C>T
NC_000012.11:g.6143978C>T
CM000674.1:g.6143978C>T
NC_000012.10:g.6014239C>T
NG_009072.1:g.94859G>A
NG_009072.2:g.94859G>A
ENST00000261405.10:c.2561G>A
ENST00000261405.9:c.2561G>A
ENST00000538635.5:n.421-40878G>A
NM_000552.3:c.2561G>A
NM_000552.4:c.2561G>A
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Pathogenic

Met criteria codes 4
PS3 PP1 PP4_Moderate PM3_Strong
Not Met criteria codes 5
BS1 BP4 PP3 PM2 PM5

Evidence Links 0

Expert Panel

Criteria Specification Information

Criteria Specification: ClinGen von Willebrand Disease Expert Panel Specifications to the ACMG/AMP Variant Interpretation Guidelines for VWF Version 1.0.0

Criteria Specification Approval History
Criteria Specifications for this VCEP
Evidence submitted by expert panel
von Willebrand Disease VCEP
The NM_000552.5(VWF):c.2561G>A variant in VWF is a missense variant predicted to cause substitution of arginine by glutamine at amino acid 854. The Grpmax filtering allele frequency in gnomAD v4.0 is 0.005857 (based on 7050/1180026 alleles, with 24 homozygotes) in the European non-Finnish population. This allele frequency is above the ClinGen VWD VCEP threshold for VWD Type 2N (<0.005) for PM2_Supporting but below the threshold (>0.01) for BS1 and therefore does not meet any population criterion. At least 9 patients with this variant displayed excessive mucocutaneous bleeding, low FVIII activity, and decreased VWF:FVIII binding, which is highly specific for VWD type 2N (PP4_Moderate, PMID: 28971901, PMID: 22875612). Four individuals were homozygous for the variant (PMID: 28971901, PMID: 22875612, PMID: 1832934) and one of those individuals was compound heterozygous for the variant and a pathogenic variant (p.Arg816Trp) confirmed in trans (PMID: 1832934), additional compound heterozygotes have been reported but were not considered here (PM3_Strong). In one family, the variant segregated with VWD type 2N in the proband and a second affected family member (PP1; PMID: 28971901). A hydrodynamic mouse model showed reduced factor VIII stability and impaired binding of factor VIII to VWF, indicating that this variant has a damaging effect on protein function (PMID: 28581694)(PS3). In summary, this variant meets the criteria to be classified as Pathogenic for von Willebrand disease type 2N. ACMG/AMP criteria applied as specified by the ClinGen von Willebrand disease Variant Curation Expert Panel: PS3, PM3_Strong, PP4_Moderate, PP1.
Met criteria codes
PS3
A hydrodynamic mouse model with wild-type and p.Arg854Gln mutant VWF proteins was generated from the plasma of VWF/FVIII double knockout mice, and p.Arg854Gln samples showed reduced factor VIII stability and impaired binding of factor VIII to VWF, indicating that this variant has a damaging effect on protein function (PMID: 28581694)(PS3).
PP1
The variant has been reported to segregate with VWD type 2N in the proband plus one affected family member (PP1; PMID: 28971901).
PP4_Moderate
At least 4 patients with this variant displayed excessive mucocutaneous bleeding (score between 6 and 16) as well as low FVIII activity (between 3 and 24) and decreased VWF:FVIII binding (between 0.02 and 0.11), which is highly specific for VWD type 2N. (PP4_Moderate, PMID: 28971901). Additional consistent phenotypes were also reported in the patients including normal HMW multimers. While NGS was used for genotyping, it is not clear whether the alternate diagnosis of Hemophilia A was successfully ruled out in these patients. Two additional homozygous affected individuals have been found in PMID: 22875612.
PM3_Strong
This variant has been detected in at least 9 individuals with VWD Type 2N. 4 individuals were homozygous for the variant (1 point maximum, PMID: 28971901, PMID: 22875612, PMID: 1832934). 1 of those individuals was compound heterozygous for the variant and a pathogenic variant (p.Arg816Trp) confirmed in trans (1 point, PMID: 1832934). Total 2pt (PM3_Strong) 2 additional individuals were compound heterozygous for the p.Arg854Gln variant with a second variant confirmed in trans (p.Arg324Ter and p.Pro2558GlyfsTer7, respectively, 2 points, PMID: 28971901) but quantitative VWD classification rules are not yet finalized.
Not Met criteria codes
BS1
The Grpmax filtering allele frequency in gnomAD v4.1 is 0.005857 (based on 7050/1180026 alleles, with 24 homozygotes) in the European non-Finnish population. This allele frequency is below the ClinGen VWD VCEP threshold (>0.01) for VWD Type 2N variants for BS1.
BP4
The computational predictor REVEL gives a score of 0.487, which is above the ClinGen VWD VCEP PP3 threshold of <0.290.
PP3
The computational predictor REVEL gives a score of 0.487, which is below the ClinGen VWD VCEP PP3 threshold of >0.644 and does not predict a damaging effect on VWF function. The computational splicing predictor SpliceAI gives a score of 0.02 for splice acceptor gain, indicating that the variant likely has no impact on splicing.
PM2
The Grpmax filtering allele frequency in gnomAD v4.1 is 0.005857 (based on 7050/1180026 alleles, with 24 homozygotes) in the European non-Finnish population. This allele frequency is above the ClinGen VWD VCEP threshold (<0.005) for VWD Type 2N variants for PM2_Supporting.
PM5
Another missense variant NM_000552.5(VWF):c.2560C>T (p.Arg854Trp) (PMID: 9684781, PMID: 20586924, ClinVar Variation ID: 100228) in the same codon has not yet been classified for VWD Type 2N by the ClinGen VWD VCEP, and PM5 will not be evaluated in this curation to avoid circularity.
Curation History
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