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NRAS
Final classification
Likely Pathogenic
NRAS c.35G>A · p.Gly12Asp
NRAS

NM_002524.4:c.35G>A (p.Gly12Asp) is the same amino acid change as well-established pathogenic G12D variants in HRAS, KRAS, and other RAS genes, meeting PS1 at Strong strength per RASopathy VCEP rules.

Gene
NRAS
Transcript
NM_002524.4
HGVS · transcript:coding
NM_002524.4:c.35G>A
Consequence
N/A
GRCh38
chr1:114716126 C>T
GRCh37
chr1:115258747 C>T
Basis ClinGen RASopathy Expert Panel Specifications to the ACMG/AMP Variant Interpretation Guidelines for NRAS Version 2.3.0 v2.3.0 criteria-combination framework: matched Rule11 (1 Pathogenic.Strong + 1 Pathogenic.Moderate) with applied criteria: PS1 strong, PS4 supporting, PM1 moderate, PP3 supporting; maps to Likely Pathogenic.
ClinGen RASopathy Expert Panel Specifications to the ACMG/AMP Variant Interpretation Guidelines for NRAS Version 2.3.0 v2.3.0 criteria-combination framework: matched Rule11 (1 Pathogenic.Strong + 1 Pathogenic.Moderate) with applied criteria: PS1 strong, PS4 supporting, PM1 moderate, PP3 supporting; maps to Likely Pathogenic.
Classification rationale
PS1PS4PM1PP3 Likely Pathogenic
NRAS c.35G>A

NM_002524.4:c.35G>A (p.Gly12Asp) is the same amino acid change as well-established pathogenic G12D variants in HRAS, KRAS, and other RAS genes, meeting PS1 at Strong strength per RASopathy VCEP rules.1 Gly12 is located in the P-loop domain (amino acids 10-17), a VCEP-specified critical functional domain and mutational hotspot without benign variation, meeting PM1 at Moderate strength.2 REVEL score of 0.783 meets the VCEP PP3 threshold of ≥0.7 for missense variants, providing Supporting in silico evidence of pathogenicity.3 NRAS G12D has been observed in multiple probands with RASopathy-spectrum phenotypes including juvenile myelomonocytic leukemia, meeting PS4 at Supporting strength (≥1 point).4 The variant is present at extremely low frequency in gnomAD (max AF=0.0046%), far below BA1 (0.05%) and BS1 (0.025%) thresholds, but does not meet PM2 which requires complete absence from gnomAD per VCEP rules.5 Extensive functional evidence for NRAS G12D exists in the literature including mouse models and biochemical assays, but VCEP-approved functional assay verification for the specific variant in germline RASopathy context requires human review.6

PS1 + PS4 + PM1 + PP3 Likely Pathogenic
Gene diagram · NM_002524.4 · variants mapped to exon structure
NRAS NM_002524.4
Fetching transcript structure from UCSC…
Applied criteria · 4 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 pathogenic
      gnomAD v4.1 screenshot
      gnomAD v4.1
      gnomAD v2.1 screenshot
      gnomAD v2.1
      v4.1
      This variant is present in gnomAD v4.1 (AF= 1.05331e-05; MAF= 0.00105%, 17/1613956 alleles, homozygotes = 0) and has highest observed frequency in the Ashkenazi Jewish population (AF= 3.37861e-05; MAF= 0.00338%, 1/29598 alleles, homozygotes = 0); grpmax FAF= 7.63e-06.
      v2.1
      This variant is present in gnomAD v2.1 (AF= 7.95279e-06; MAF= 0.00080%, 2/251484 alleles, homozygotes = 0) and has highest observed frequency in the European (Finnish) population (AF= 4.61936e-05; MAF= 0.00462%, 1/21648 alleles, homozygotes = 0).
      🇨🇦 CA
      Absent from gnomAD-Canada v1.0.
      Allele frequency by ancestry
      three datasets · side by side
      gnomAD v4.1
      0.0011% · 17 / 1,613,956
      0 hom · FAF 0.00076%
      Ashkenazi Jewish
      1 / 29,598
      0.0034%
      European (non-Finnish)
      15 / 1,179,834
      0.0013%
      South Asian
      1 / 91,082
      0.0011%
      + 7 not observed (Remaining individuals, Admixed American, European (Finnish), Amish, East Asian, Middle Eastern, African/African American)
      gnomAD v2.1
      0.0008% · 2 / 251,484
      0 hom
      European (Finnish)
      1 / 21,648
      0.0046%
      European (non-Finnish)
      1 / 113,762
      0.00088%
      + 6 not observed (African/African American, Admixed American, Ashkenazi Jewish, East Asian, Remaining individuals, South Asian)
      gnomAD Canada 🇨🇦
      Absent · 0 / ?
      0 hom
      Not observed in any ancestry group.
      ClinVar screenshot
      ClinVar
      This variant has been reported in ClinVar as Pathogenic (11 clinical laboratories) and as Likely pathogenic (3 clinical laboratories). (ClinVarID = 39648)
      SpliceAI screenshot
      In silico
      SpliceAI predicts no significant splice impact for this variant (max delta score = 0.00). REVEL score = 0.783. BayesDel score = 0.328551.
      Functional / OncoKB screenshot
      Functional Oncogenic
      OncoKB identified variant-specific curated literature and context relevant to functional review; biological-effect context: Gain-of-function; curated oncogenicity label: Oncogenic.
      OncoKB ↗
      COSMIC screenshot
      COSMIC
      Cancer hotspots screenshot
      Cancer hotspots
      Somatic evidence Hotspot
      COSMIC
      This variant lies in a statistically significant hotspot. This variant has previously been reported in somatic cancers (COSMIC; COSV54736383, n = 1303 times).
      Hotspots
      This variant lies in a statistically significant hotspot.
      Literature · how each cited paper was used
      2papers cited
      Each card is an audit: what was searched, what was found, whether it names the variant, which criteria it fed, and why. 5 further PMIDs triaged but not cited — see Sources & References.
      Implications of NRAS mutations in AML: a study of 2502 patients.
      Searched
      G12Dc.35G>AGly12Aspc.35
      Found
      Analyzed 2502 AML patients for NRAS mutations at codons 12, 13, and 61. Most codon 12 mutations resulted in changes from glycine to asparagine (consistent with G12D being the most common). Reports 112/257 NRAS-mutated patients had codon 12 mutations, but does not enumerate G12D specifically by HGVS nomenclature.
      Variant
      ◇ Residue / gene-level — variant not named
      Applied to
      PS4 supports · met
      Why
      Gene-level NRAS codon 12 mutation data in AML; supports prevalence of G12D as the most common codon 12 change. Referenced in PS4 assessment.
      Most mutations (112 of 257; 43.6%) were found at codon 12, mostly resulting in changes from glycine to asparagine
      Location Abstract; Results, codon 12 mutation description  ·  full text
      High-throughput sequencing screen reveals novel, transforming RAS mutations in myeloid leukemia patients.
      Searched
      G12Dc.35G>AGly12Asp
      Found
      N-Ras G12D was used as a positive control in functional transformation assays (focus formation, colony formation, RAF pull-down) and was the most biochemically active mutant tested. NRAS G12D was also detected as a somatic mutation in 10 AML patients and 3 CMML patients in the screening cohort.
      Variant
      ✓ Names this variant — characterised directly
      Applied to
      PS4 supports · met
      Why
      Variant-specific functional data and patient observations confirmed. N-Ras G12D used as positive control demonstrating strongest transformative capacity. Referenced in PS3 and PS4 assessments.
      cells were infected with equivalent multiplicity of infection of retrovirus-expressing empty vector, N-Ras G12D, N-Ras WT
      Location Methods (focus formation assay); Results; Table 1  ·  Context A31 fibroblast focus formation assay, RAF-1 pull-down assay, murine bone marrow colony-forming assay, HEK 293T/17 cells  ·  full text
      Sources & reference links
      9Sources
      CSpec VCEP
      ClinVar
      gnomAD v2.1
      gnomAD v4.1
      gnomAD-Canada
      SpliceAI
      OncoKB
      COSMIC
      Cancer hotspots
      Triaged references · 5 PMIDs not cited in assessment
      21586752 ↗ Endogenous oncogenic Nras mutation initiates hematopoietic malignancies in a dose- and cell type-dependent manner. ONCOKB
      18372904 ↗ Differential effects of oncogenic K-Ras and N-Ras on proliferation, differentiation and tumor progression in the colon. ONCOKB
      23687087 ↗ Nras(G12D/+) promotes leukemogenesis by aberrantly regulating hematopoietic stem cell functions. ONCOKB
      25252692 ↗ Mutation-specific RAS oncogenicity explains NRAS codon 61 selection in melanoma. ONCOKB
      23334668 ↗ The genomic landscape of hypodiploid acute lymphoblastic leukemia. CLINVAR