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POLE
Final classification
VUS
POLE c.4189C>A · p.Leu1397Ile
POLE

NM_006231.3:c.4189C>A (p.Leu1397Ile) is absent from gnomAD v2.1, v4.1, and gnomAD-Canada, meeting PM2 at Supporting strength.

Gene
POLE
Transcript
NM_006231.3
HGVS · transcript:coding
NM_006231.3:c.4189C>A
Consequence
N/A
GRCh38
chr12:132643938 G>T
GRCh37
chr12:133220524 G>T
Basis Only one criterion is met: PM2 at Supporting strength (absent from gnomAD v2.1, v4.1, and gnomAD-Canada). No pathogenic, likely pathogenic, benign, or likely benign combination threshold is satisfied under ACMG/AMP 2015 rules. Per the León-Castillo et al. 2020 custom POLE framework, criterion triggering and strength are customized (PM1, PS4, PP3, BP4), but final classification combination follows standard ACMG/AMP 2015 thresholds, which explicitly state that all other combinations default to VUS.
Only one criterion is met: PM2 at Supporting strength (absent from gnomAD v2.1, v4.1, and gnomAD-Canada). No pathogenic, likely pathogenic, benign, or likely benign combination threshold is satisfied under ACMG/AMP 2015 rules. Per the León-Castillo et al. 2020 custom POLE framework, criterion triggering and strength are customized (PM1, PS4, PP3, BP4), but final classification combination follows standard ACMG/AMP 2015 thresholds, which explicitly state that all other combinations default to VUS.
Classification rationale
PM2 VUS
POLE c.4189C>A

NM_006231.3:c.4189C>A (p.Leu1397Ile) is absent from gnomAD v2.1, v4.1, and gnomAD-Canada, meeting PM2 at Supporting strength.1 No other pathogenic or benign criteria are met. The variant is a C-terminal missense change outside the exonuclease domain, with no functional data, no clinical observations, no segregation data, and indeterminate computational predictions (REVEL 0.329, BayesDel -0.262).2 With only PM2_Supporting met, the evidence is insufficient to classify this variant as pathogenic or likely pathogenic, and insufficient to classify as benign or likely benign. This variant is classified as a Variant of Uncertain Significance (VUS) per ACMG/AMP 2015 guidelines.3

PM2 VUS
3 generic_acmg_combination_rules
Gene diagram · NM_006231.3 · variants mapped to exon structure
POLE NM_006231.3
Fetching transcript structure from UCSC…
Applied criteria · 1 applied · 21 assessed
Applied · 1
Strength Supporting Moderate Strong Very strong
PM2 supporting Pathogenic
NM_006231.3:c.4189C>A (p.Leu1397Ile) is absent from gnomAD v2.1, gnomAD v4.1, and gnomAD-Canada v1.0, indicating it is not observed in large population cohorts.
Absent from gnomAD v2.1 (0 alleles)gnomAD v4.1 (0 alleles)and gnomAD-Canada v1.0 (0 alleles).
Assessed · not applied
Pathogenic
PS1 No pathogenic missense variant has been identified at codon 1397.
PS2 No de novo observations have been reported for NM_006231.3:c.4189C>A.
PS3 No functional studies have been performed on p.Leu1397Ile or a systematically characterized range that includes residue 1397.
PS4 The variant is absent from the León-Castillo Supplementary Table S1 and is not recurrent in COSMIC or TCGA endometrial carcinoma cohorts.
PM1 Residue 1397 is in the C-terminal region of POLE, well outside the exonuclease domain (residues ~268–471).
PM6 No de novo observations of NM_006231.3:c.4189C>A have been reported.
PP1 No segregation data are available for NM_006231.3:c.4189C>A.
PP2 No HCI prior score is available for this variant.
PP3 The variant is absent from León-Castillo Supplementary Tables S2 and S3, so the custom PP3_Supporting rule does not apply.
PP4 No clinical phenotype data are available for NM_006231.3:c.4189C>A.
PP5 No reputable source has classified NM_006231.3:c.4189C>A as pathogenic.
Benign
BA1 The variant is absent from gnomAD v2.1, v4.1, and gnomAD-Canada.
BS1 The variant is absent from all population databases.
BS2 No homozygous or compound heterozygous observations of NM_006231.3:c.4189C>A have been reported.
BS3 No functional studies have been performed demonstrating a benign effect for p.Leu1397Ile.
BS4 No segregation or family data are available for NM_006231.3:c.4189C>A.
BP1 Although this is a missense variant, POLE disease mechanism is not restricted to loss-of-function/truncating variants.
BP2 No co-occurrence data are available.
BP4 The variant is absent from León-Castillo Supplementary Tables S2 and S3, so the custom BP4_Supporting rule does not apply.
BP5 No reputable source has classified NM_006231.3:c.4189C>A as benign.
BP6 No reputable source has classified NM_006231.3:c.4189C>A as benign.
N/A · 3 PVS1 · PM5 · 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 = 0.01). REVEL score = 0.329. BayesDel score = -0.262205.
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. POLE, the catalytic subunit of DNA polymerase epsilon, is an enzyme involved in DNA replication and repair. Select POLE mutations lead to ultra-high m
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