Starting

Initialising…

KRAS

Final classification

Likely Pathogenic

KRAS c.179G>T · p.Gly60Val

KRAS

NM_033360.3:c.179G>T (p.Gly60Val) is a missense variant in KRAS identified in a single de novo proband with Noonan syndrome and lethal hypertrophic cardiomyopathy (Nosan et al. 2013).

Gene

KRAS

Transcript

NM_033360.3

HGVS · transcript:coding

NM_033360.3:c.179G>T

Consequence

N/A

GRCh38

chr12:25227345 C>A

GRCh37

chr12:25380279 C>A

Basis ClinGen RASopathy Expert Panel Specifications to the ACMG/AMP Variant Interpretation Guidelines for KRAS Version 2.3.0 v2.3.0 criteria-combination framework: matched Rule13 (Pathogenic.Moderate >=3) with applied criteria: PS2 moderate, PS4 supporting, PM1 moderate, PM5 moderate, PP3 supporting; maps to Likely Pathogenic. ▾

ClinGen RASopathy Expert Panel Specifications to the ACMG/AMP Variant Interpretation Guidelines for KRAS Version 2.3.0 v2.3.0 criteria-combination framework: matched Rule13 (Pathogenic.Moderate >=3) with applied criteria: PS2 moderate, PS4 supporting, PM1 moderate, PM5 moderate, PP3 supporting; maps to Likely Pathogenic.

Classification rationale

PS2PS4PM1PM5PP3 Likely Pathogenic

KRAS c.179G>T

NM_033360.3:c.179G>T (p.Gly60Val) is a missense variant in KRAS identified in a single de novo proband with Noonan syndrome and lethal hypertrophic cardiomyopathy (Nosan et al. 2013).¹ The variant affects Gly60, which resides in the Switch II domain (AA 57–64), a critical functional domain per RASopathy VCEP specifications (PM1_Moderate).² At least two different pathogenic missense changes (p.Gly60Ser, p.Gly60Arg) have been reported at the same codon in RASopathy patients, satisfying PM5 at Moderate strength.³ Parental genotyping confirmed the variant occurred de novo, meeting PS2 at Moderate strength (1 de novo point per VCEP rules).⁴ The variant is observed in a single RASopathy proband, meeting PS4 at Supporting strength (≥1 point per VCEP rules).⁵ REVEL in silico score of 0.879 exceeds the VCEP threshold of ≥0.7, meeting PP3 at Supporting strength.⁶ The variant is present at extremely low frequency in gnomAD (v2.1: 1/251,328; v4.1: 3/1,614,068), which is below benign population thresholds but above the PM2 absence requirement.⁷ Applying the RASopathy VCEP classification rules: three Moderate criteria (PS2_Moderate, PM1, PM5) plus two Supporting criteria (PS4_Supporting, PP3) are met. Per VCEP Rule13, ≥3 Moderate criteria yields a classification of Likely Pathogenic.⁸

PS2 + PS4 + PM1 + PM5 + PP3 → Likely Pathogenic

1 PMID:24382853 ↗

2 cspec ↗

3 PMID:24382853 ↗

4 PMID:24382853 ↗

5 PMID:24382853 ↗

6 revel

7 gnomad_v2 ↗gnomad_v4 ↗

8 cspec ↗

Gene diagram · NM_033360.3 · variants mapped to exon structure

KRAS NM_033360.3

Fetching transcript structure from UCSC…

Applied criteria · 5 met · select any tile

Met

Not met

Not assessed

N/A

Strength very strong supporting

Pathogenic evidence

PVS

Benign evidence

—

Rationale

Select a criterion.

Sources

Evidence used

Gaps remaining

Rule

—

Research & evidence

Population frequency · supports pathogenic

gnomAD v4.1

gnomAD v2.1

v4.1

This variant is present in gnomAD v4.1 (AF= 1.85866e-06; MAF= 0.00019%, 3/1614068 alleles, homozygotes = 0) and has highest observed frequency in the European (non-Finnish) population (AF= 2.54241e-06; MAF= 0.00025%, 3/1179982 alleles, homozygotes = 0); grpmax FAF= 6.8e-07.

v2.1

This variant is present in gnomAD v2.1 (AF= 3.97886e-06; MAF= 0.00040%, 1/251328 alleles, homozygotes = 0) and has highest observed frequency in the European (non-Finnish) population (AF= 8.79879e-06; MAF= 0.00088%, 1/113652 alleles, homozygotes = 0).

🇨🇦 CA

Absent from gnomAD-Canada v1.0.

Allele frequency by ancestry

three datasets · side by side

gnomAD v4.1

0.00019% · 3 / 1,614,068
0 hom · FAF 6.8e-05%

European (non-Finnish)

3 / 1,179,982

0.00025%

+ 9 not observed (Remaining individuals, Admixed American, European (Finnish), Amish, East Asian, Middle Eastern, South Asian, Ashkenazi Jewish, African/African American)

gnomAD v2.1

0.0004% · 1 / 251,328
0 hom

European (non-Finnish)

1 / 113,652

0.00088%

+ 7 not observed (African/African American, Admixed American, Ashkenazi Jewish, East Asian, European (Finnish), Remaining individuals, South Asian)

gnomAD Canada 🇨🇦

Absent · 0 / ?
0 hom

Not observed in any ancestry group.

gnomAD v4 ↗ gnomAD v2 ↗ gnomAD 🇨🇦 ↗

ClinVar

This variant has been reported in ClinVar as Pathogenic (4 clinical laboratories) and as Likely pathogenic (3 clinical laboratories). (ClinVarID = 163766)

ClinVar ↗

In silico

SpliceAI predicts possible splice impact for this variant (max delta score = 0.25). REVEL score = 0.879. BayesDel score = 0.303486.

SpliceAI ↗

Functional Likely Oncogenic

OncoKB identified variant-specific curated literature and context relevant to functional review; biological-effect context: Likely Gain-of-function; curated oncogenicity label: Likely Oncogenic.

OncoKB ↗

COSMIC

Cancer hotspots

Somatic evidence Hotspot

COSMIC

This variant lies in a statistically significant hotspot. This variant has previously been reported in somatic cancers (COSMIC; COSV55708344, n = 5 times).

Hotspots

This variant lies in a statistically significant hotspot.

COSMIC ↗ Hotspots ↗

Literature · how each cited paper was used

1papers cited

Each card is an audit: what was searched, what was found, whether it names the variant, which criteria it fed, and why. 7 further PMIDs triaged but not cited — see Sources & References.

A lethal course of hypertrophic cardiomyopathy in Noonan syndrome due to a novel germline mutation in the KRAS gene: case study.

PMID 24382853 ↗ · Nosan G et al. · 2013 Dec CLINVAR · functional

Searched

c.179G>Tp.Gly60ValG60VGly60Val179G>T

Found

A heterozygous missense variant c.179G>T (p.Gly60Val) in KRAS exon 3 was identified as a de novo germline mutation in a preterm infant with Noonan syndrome, dysmorphic features, and rapidly progressive hypertrophic cardiomyopathy leading to death at 4 months of age. The authors note that other mutations at the same residue (p.Gly60Ser, p.Gly60Arg) are known pathogenic NS variants.

Variant

✓ Names this variant — characterised directly

Applied to

→PM5 supports · met →PS2 supports · met →PS4 supports · met

Why

Variant-specific germline case with confirmed de novo status; referenced for PS2_Moderate, PS4_Supporting, and PM5_Moderate adjudications.

This heterozygous unclassified missense variant in exon 3: c.179G>T (p.Gly60Val) might be associated with a lethal form of Noonan syndrome.

Location Abstract; Case Report, paragraph 2; Discussion, paragraphs 1-2; Figure 2 · Context Clinical case report; Sanger sequencing of KRAS coding exons; parental DNA genotyping confirmed de novo status · full text

Sources & reference links

9Sources

CSpec VCEP

ClinVar

gnomAD v2.1

gnomAD v4.1

gnomAD-Canada

SpliceAI

OncoKB

COSMIC

Cancer hotspots

Triaged references · 7 PMIDs not cited in assessment

24446311 ↗ BRAF kinase domain mutations are present in a subset of chronic myelomonocytic leukemia with wild-type RAS. ONCOKB

27288520 ↗ Spectrum and prognostic relevance of driver gene mutations in acute myeloid leukemia. ONCOKB

34117033 ↗ Clinical and Functional Characterization of Atypical KRAS/NRAS Mutations in Metastatic Colorectal Cancer. ONCOKB

19396835 ↗ Craniosynostosis in patients with Noonan syndrome caused by germline KRAS mutations. CLINVAR

30813707 ↗ Provisional Guideline Recommendation for EGFR Gene Mutation Testing in Liquid Samples of Lung Cancer Patients: A Proposal by the Korean Cardiopulmonary Pathology Study Group. CLINVAR

34958143 ↗ Trio exome sequencing is highly relevant in prenatal diagnostics. CLINVAR

16474404 ↗ Germline KRAS and BRAF mutations in cardio-facio-cutaneous syndrome. CLINVAR