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KDR
Final classification
VUS
KDR c.3247A>T · p.Thr1083Ser
KDR

NM_002253.3:c.3247A>T (p.Thr1083Ser) in KDR is a missense variant in exon 24. It is completely absent from gnomAD v2.1, v4.1, and gnomAD-Canada, meeting PM2 at supporting level.

Gene
KDR
Transcript
NM_002253.3
HGVS · transcript:coding
NM_002253.3:c.3247A>T
Consequence
N/A
GRCh38
chr4:55089748 T>A
GRCh37
chr4:55955915 T>A
Basis gene-specific framework lacked a usable explicit final combination framework, so generic ACMG/AMP 2015 final-combination rules were applied as fallback; applied criteria: PM2 supporting; combination = 1 supporting, which maps to VUS.
gene-specific framework lacked a usable explicit final combination framework, so generic ACMG/AMP 2015 final-combination rules were applied as fallback; applied criteria: PM2 supporting; combination = 1 supporting, which maps to VUS.
Classification rationale
PM2 VUS
KDR c.3247A>T

NM_002253.3:c.3247A>T (p.Thr1083Ser) in KDR is a missense variant in exon 24. It is completely absent from gnomAD v2.1, v4.1, and gnomAD-Canada, meeting PM2 at supporting level.1 No variant-specific functional studies, case-control data, family segregation data, or de novo observations are available. The variant is absent from ClinVar and has not been reported in any peer-reviewed publication.2 Computational predictors are conflicting: REVEL 0.638 suggests a deleterious effect, while BayesDel -0.0950088 predicts benign, and SpliceAI shows no splicing impact (max delta = 0.00). PP3 and BP4 are not met.3 The only applicable criterion is PM2 (supporting). Under generic ACMG/AMP 2015 combination rules (PMID:25741868), a single supporting criterion is insufficient to classify the variant as likely pathogenic or likely benign. The variant defaults to a classification of Uncertain Significance.4

PM2 VUS
3 revelbayesdelspliceai ↗
4 generic_acmg_combination_rules
Gene diagram · NM_002253.3 · variants mapped to exon structure
KDR NM_002253.3
Fetching transcript structure from UCSC…
Applied criteria · 1 applied · 20 assessed
Applied · 1
Strength Supporting Moderate Strong Very strong
PM2 supporting Pathogenic
NM_002253.3:c.3247A>T is completely absent from gnomAD v2.1 (exomes), gnomAD v4.1 (exomes), and gnomAD-Canada v1.0 (genomes). This meets the non-VCEP PM2 threshold of allele frequency <0.1%.
Absent from gnomAD v2.1 (AC=0).Absent from gnomAD v4.1 (AC=0).Absent from gnomAD-Canada v1.0 (AC=0).
Assessed · not applied
Pathogenic
PS1 No alternative nucleotide change at c.3247 resulting in p.Thr1083Ser has been established as pathogenic.
PS2 No de novo observation with confirmed paternity and maternity has been reported for NM_002253.3:c.3247A>T in any available source.
PS3 No well-established in vitro or in vivo functional studies have been identified for p.Thr1083Ser.
PS4 No case-control data or cohort enrichment data are available for this variant.
PM1 The variant does not lie in a statistically significant mutational hotspot (Cancer Hotspots negative).
PM6 No de novo observation (with or without confirmed parentage) has been reported for this variant in any available source.
PP1 No cosegregation data available for this variant; no family studies identified in any evidence source.
PP2 No gene-level constraint data (missense Z-score, HCI prior) are available for KDR to determine whether the gene has a low rate of benign missense variation.
PP3 Computational evidence is conflicting.
PP4 No patient phenotype or clinical data are available to evaluate whether the proband's features are highly specific for a KDR-related disorder.
Benign
BA1 Variant is absent from all population databases.
BS1 Variant is absent from all population databases.
BS2 No observation of this variant in a homozygous state in healthy adults or at high allele frequency in a recessive disease context.
BS3 No well-established functional studies demonstrating a benign or neutral effect have been identified for p.Thr1083Ser.
BS4 No segregation or nonsegregation data available.
BP1 While KDR loss of function is supported as a germline disease mechanism by targeted literature review, there is insufficient evidence to conclude that only truncating variants cause disease and that missense variants are not pathogenic.
BP2 No observation of this variant in trans with a known pathogenic variant in KDR.
BP4 Computational evidence is conflicting and does not provide multiple lines of support for a benign interpretation.
BP5 No observation of this variant in an individual with an alternate molecular cause for disease.
BP6 This variant has not been reported as benign by a reputable source.
N/A · 4 PVS1 · PM5 · PP5 · BP7
Research & evidence
Population frequency
gnomAD v4.1 screenshot
gnomAD v4.1
gnomAD v2.1 screenshot
gnomAD v2.1
v4.1
Absent from gnomAD v4.1.
v2.1
Absent from gnomAD v2.1.
🇨🇦 CA
Absent from gnomAD-Canada v1.0.
Allele frequency by ancestry
three datasets · side by side
gnomAD v4.1
Absent · 0 / ?
0 hom
Not observed in any ancestry group.
gnomAD v2.1
Absent · 0 / ?
0 hom
Not observed in any ancestry group.
gnomAD Canada 🇨🇦
Absent · 0 / ?
0 hom
Not observed in any ancestry group.
ClinVar screenshot
ClinVar
This variant is absent from ClinVar.
SpliceAI screenshot
In silico
SpliceAI predicts no significant splice impact for this variant (max delta score = 0.00). REVEL score = 0.638. BayesDel score = -0.0950088.
Functional / OncoKB screenshot
Functional Unknown Oncogenic Effect
OncoKB did not identify variant-specific reviewed functional evidence for this variant; gene-level curated context is available for reviewer follow-up. KDR, a receptor tyrosine kinase, is altered by mutation or amplification in various cancers, most frequently in skin cancers.
OncoKB ↗
COSMIC screenshot
COSMIC
Cancer hotspots screenshot
Cancer hotspots
Somatic evidence Not in COSMIC / hotspots
COSMIC
This variant does not lie in a statistically significant hotspot. This variant has not previously been reported in somatic cancers (COSMIC).
Hotspots
This variant does not lie in a statistically significant hotspot.
Sources & reference links
8Sources
ClinVar
gnomAD v2.1
gnomAD v4.1
gnomAD-Canada
SpliceAI
OncoKB
COSMIC
Cancer hotspots