Classification rationale

BS1BP4BP7 Likely Benign

EZHIP c.1272G>A

NM_203407.3:c.1272G>A (p.Gln424=) is a synonymous variant in EZHIP exon 1. SpliceAI predicts no splicing impact (max delta=0.02), consistent with a silent substitution.¹ This variant is present in gnomAD v2.1 with a grpmax filtering allele frequency of 0.47% (82/204,972 alleles, 1 homozygote) and an East Asian subpopulation frequency of 0.54% (80/14,835 alleles, 1 homozygote), exceeding the 0.3% threshold expected for a rare disease variant and supporting a benign interpretation.² The variant is absent from ClinVar and has not been reported in the published literature. No functional studies, segregation data, or case-control evidence exists to support pathogenicity.³ No pathogenic criteria are met. Benign evidence includes BS1 (supporting benign; population frequency), BP4 (supporting benign; in silico predictions), and BP7 (supporting benign; synonymous with silent splice prediction). Overall, the variant is classified as Likely Benign.⁴

BS1 + BP4 + BP7 → Likely Benign

1 spliceai ↗

2 gnomad_v2 ↗

3 clinvar ↗

4 gnomad_v2 ↗spliceai ↗

Gene diagram · NM_203407.3 · variants mapped to exon structure

EZHIP NM_203407.3

Fetching transcript structure from UCSC…

Applied criteria · 3 met · select any tile

Met

Not met

Not assessed

N/A

Strength very strong supporting

Pathogenic evidence

PVS

PS

PM

PP

Benign evidence

BA

BS

BP

—

Rationale

Select a criterion.

Sources

Evidence used

Gaps remaining

Rule

—

Research & evidence

Population frequency · supports benign

gnomAD v4.1

gnomAD v2.1

v4.1

This variant is present in gnomAD v4.1 (AF= 0.000142255; MAF= 0.01423%, 81/569401 alleles, homozygotes = 1) and has highest observed frequency in the East Asian population (AF= 0.00234497; MAF= 0.23450%, 72/30704 alleles, homozygotes = 1); grpmax FAF= 0.00190909.

v2.1

This variant is present in gnomAD v2.1 (AF= 0.000400055; MAF= 0.04001%, 82/204972 alleles, homozygotes = 1) and has highest observed frequency in the East Asian population (AF= 0.00539265; MAF= 0.53927%, 80/14835 alleles, homozygotes = 1); grpmax FAF= 0.00468821.

🇨🇦 CA

This variant is present in gnomAD-Canada v1.0 (AF= 0.000414651002073255, 6/14470 alleles, homozygotes = 0).

Allele frequency by ancestry

three datasets · side by side

gnomAD v4.1

0.014% · 81 / 569,401
1 hom · FAF 0.19%

East Asian 72 / 30,704	0.23% 1 hom
Remaining individuals 7 / 26,445	0.026%
South Asian 1 / 44,788	0.0022%
Admixed American 1 / 45,068	0.0022%

+ 6 not observed (European (Finnish), Amish, Middle Eastern, Ashkenazi Jewish, African/African American, European (non-Finnish))

gnomAD v2.1

0.04% · 82 / 204,972
1 hom · FAF 0.47%

East Asian 80 / 14,835	0.54% 1 hom
Remaining individuals 1 / 5,334	0.019%
South Asian 1 / 19,053	0.0052%

+ 5 not observed (African/African American, Admixed American, Ashkenazi Jewish, European (Finnish), European (non-Finnish))

gnomAD Canada 🇨🇦

0.041% · 6 / 14,470
0 hom · FAF 0.25%

East Asian

6 / 1,040

0.58%

+ 8 not observed (African/African American, Latino/Admixed American, Ashkenazi Jewish, European (Finnish), Middle Eastern, European (non-Finnish), Remaining individuals, South Asian)

gnomAD v4 ↗ gnomAD v2 ↗ gnomAD 🇨🇦 ↗

ClinVar

This variant is absent from ClinVar.

ClinVar ↗

In silico

SpliceAI predicts no significant splice impact for this variant (max delta score = 0.02).

SpliceAI ↗

Functional Unknown Oncogenic Effect

OncoKB identified curated literature and non-variant-specific oncogenicity context for review; listed oncogenicity label: Unknown Oncogenic Effect.

OncoKB ↗

COSMIC

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.

COSMIC ↗ Hotspots ↗

Sources & reference links

8Sources

ClinVar

gnomAD v2.1

gnomAD v4.1

gnomAD-Canada

SpliceAI

OncoKB

COSMIC

Cancer hotspots