dbSNP Short Genetic Variations
Welcome to the Reference SNP (rs) Report
All alleles are reported in the Forward orientation. Click on the Variant Details tab for details on Genomic Placement, Gene, and Amino Acid changes. HGVS names are in the HGVS tab.
Reference SNP (rs) Report
This page reports data for a single dbSNP Reference SNP variation (RefSNP or rs) from the new redesigned dbSNP build.
Top of the page reports a concise summary for the rs, with more specific details included in the corresponding tabs below.
All alleles are reported in the Forward orientation. Use the Genomic View to inspect the nucleotides flanking the variant, and its neighbors.
For more information see Help documentation.
rs121434595
Current Build 157
Released September 3, 2024
- Organism
- Homo sapiens
- Position
-
chr1:114716124 (GRCh38.p14) Help
The anchor position for this RefSNP. Includes all nucleotides potentially affected by this change, thus it can differ from HGVS, which is right-shifted. See here for details.
- Alleles
- C>A / C>G / C>T
- Variation Type
- SNV Single Nucleotide Variation
- Frequency
-
None
- Clinical Significance
- Reported in ClinVar
- Gene : Consequence
- NRAS : Missense Variant
- Publications
- 12 citations
- Genomic View
- See rs on genome
Frequency tab displays a table of the reference and alternate allele frequencies reported by various studies and populations. Table lines, where Population="Global" refer to the entire study population, whereas lines, where Group="Sub", refer to a study-specific population subgroupings (i.e. AFR, CAU, etc.), if available. Frequency for the alternate allele (Alt Allele) is a ratio of samples observed-to-total, where the numerator (observed samples) is the number of chromosomes in the study with the minor allele present (found in "Sample size", where Group="Sub"), and the denominator (total samples) is the total number of all chromosomes in the study for the variant (found in "Sample size", where Group="Study-wide" and Population="Global").
Variant Details tab shows known variant placements on genomic sequences: chromosomes (NC_), RefSeqGene, pseudogenes or genomic regions (NG_), and in a separate table: on transcripts (NM_) and protein sequences (NP_). The corresponding transcript and protein locations are listed in adjacent lines, along with molecular consequences from Sequence Ontology. When no protein placement is available, only the transcript is listed. Column "Codon[Amino acid]" shows the actual base change in the format of "Reference > Alternate" allele, including the nucleotide codon change in transcripts, and the amino acid change in proteins, respectively, allowing for known ribosomal slippage sites. To view nucleotides adjacent to the variant use the Genomic View at the bottom of the page - zoom into the sequence until the nucleotides around the variant become visible.
| Sequence name | Change |
|---|---|
| GRCh38.p14 chr 1 | NC_000001.11:g.114716124C>A |
| GRCh38.p14 chr 1 | NC_000001.11:g.114716124C>G |
| GRCh38.p14 chr 1 | NC_000001.11:g.114716124C>T |
| GRCh37.p13 chr 1 | NC_000001.10:g.115258745C>A |
| GRCh37.p13 chr 1 | NC_000001.10:g.115258745C>G |
| GRCh37.p13 chr 1 | NC_000001.10:g.115258745C>T |
| NRAS RefSeqGene (LRG_92) | NG_007572.1:g.5771G>T |
| NRAS RefSeqGene (LRG_92) | NG_007572.1:g.5771G>C |
| NRAS RefSeqGene (LRG_92) | NG_007572.1:g.5771G>A |
| Molecule type | Change | Amino acid[Codon] | SO Term |
|---|---|---|---|
| NRAS transcript | NM_002524.5:c.37G>T | G [GGT] > C [TGT] | Coding Sequence Variant |
| GTPase NRas | NP_002515.1:p.Gly13Cys | G (Gly) > C (Cys) | Missense Variant |
| NRAS transcript | NM_002524.5:c.37G>C | G [GGT] > R [CGT] | Coding Sequence Variant |
| GTPase NRas | NP_002515.1:p.Gly13Arg | G (Gly) > R (Arg) | Missense Variant |
| NRAS transcript | NM_002524.5:c.37G>A | G [GGT] > S [AGT] | Coding Sequence Variant |
| GTPase NRas | NP_002515.1:p.Gly13Ser | G (Gly) > S (Ser) | Missense Variant |
Clinical Significance tab shows a list of clinical significance entries from ClinVar associated with the variation, per allele. Click on the RCV accession (i.e. RCV000001615.2) or Allele ID (i.e. 12274) to access full ClinVar report.
| ClinVar Accession | Disease Names | Clinical Significance |
|---|---|---|
| RCV000445167.1 | Melanoma | Pathogenic |
| ClinVar Accession | Disease Names | Clinical Significance |
|---|---|---|
| RCV000014913.5 | Carcinoma of colon | Pathogenic |
| RCV000114743.4 | Large congenital melanocytic nevus | Pathogenic |
| RCV000419545.1 | Medulloblastoma | Likely-Pathogenic |
| RCV000419583.1 | Transitional cell carcinoma of the bladder | Likely-Pathogenic |
| RCV000424942.1 | Melanoma | Pathogenic |
| RCV000426328.1 | Multiple myeloma | Likely-Pathogenic |
| RCV000427817.1 | Gastric adenocarcinoma | Likely-Pathogenic |
| RCV000428963.1 | Myelodysplastic syndrome | Likely-Pathogenic |
| RCV000434327.1 | Neoplasm of the large intestine | Likely-Pathogenic |
| RCV000437450.1 | Non-Hodgkin lymphoma | Likely-Pathogenic |
| RCV000438070.2 | Acute myeloid leukemia | Pathogenic-Likely-Pathogenic |
| RCV000444449.1 | Malignant melanoma of skin | Likely-Pathogenic |
| RCV001781267.4 | Noonan syndrome 6 | Likely-Pathogenic |
| ClinVar Accession | Disease Names | Clinical Significance |
|---|---|---|
| RCV000436341.1 | Neoplasm of stomach | Likely-Pathogenic |
Aliases tab displays HGVS names representing the variant placements and allele changes on genomic, transcript and protein sequences, per allele. HGVS name is an expression for reporting sequence accession and version, sequence type, position, and allele change. The column "Note" can have two values: "diff" means that there is a difference between the reference allele (variation interval) at the placement reported in HGVS name and the reference alleles reported in other HGVS names, and "rev" means that the sequence of this variation interval at the placement reported in HGVS name is in reverse orientation to the sequence(s) of this variation in other HGVS names not labeled as "rev".
| Placement | C= | A | G | T |
|---|---|---|---|---|
| GRCh38.p14 chr 1 | NC_000001.11:g.114716124= | NC_000001.11:g.114716124C>A | NC_000001.11:g.114716124C>G | NC_000001.11:g.114716124C>T |
| GRCh37.p13 chr 1 | NC_000001.10:g.115258745= | NC_000001.10:g.115258745C>A | NC_000001.10:g.115258745C>G | NC_000001.10:g.115258745C>T |
| NRAS RefSeqGene (LRG_92) | NG_007572.1:g.5771= | NG_007572.1:g.5771G>T | NG_007572.1:g.5771G>C | NG_007572.1:g.5771G>A |
| NRAS transcript | NM_002524.5:c.37= | NM_002524.5:c.37G>T | NM_002524.5:c.37G>C | NM_002524.5:c.37G>A |
| NRAS transcript | NM_002524.4:c.37= | NM_002524.4:c.37G>T | NM_002524.4:c.37G>C | NM_002524.4:c.37G>A |
| GTPase NRas | NP_002515.1:p.Gly13= | NP_002515.1:p.Gly13Cys | NP_002515.1:p.Gly13Arg | NP_002515.1:p.Gly13Ser |
Submissions tab displays variations originally submitted to dbSNP, now supporting this RefSNP cluster (rs). We display Submitter handle, Submission identifier, Date and Build number, when the submission appeared for the first time. Direct submissions to dbSNP have Submission ID in the form of an ss-prefixed number (ss#). Other supporting variations are listed in the table without ss#.
| No | Submitter | Submission ID | Date (Build) |
|---|---|---|---|
| 1 | OMIM-CURATED-RECORDS | ss256302352 | Aug 26, 2010 (132) |
| 2 | DF-BWCC | ss275515078 | Nov 22, 2010 (133) |
| 3 | DF-BWCC | ss275515080 | Nov 22, 2010 (133) |
| 4 | DF-BWCC | ss275515081 | Nov 22, 2010 (133) |
| 5 | EVA | ss6403965963 | Nov 02, 2024 (157) |
| 6 | GNOMAD | ss6408181591 | Nov 02, 2024 (157) |
| 7 | GNOMAD | ss6408181592 | Nov 02, 2024 (157) |
| 8 | CSS-BFX | ss8442107653 | Nov 02, 2024 (157) |
| 9 | CSS-BFX | ss8442107654 | Nov 02, 2024 (157) |
| 10 | CSS-BFX | ss8442107655 | Nov 02, 2024 (157) |
| 11 | EVA | ss8799401649 | Nov 02, 2024 (157) |
| 12 | EVA | ss8935520788 | Nov 02, 2024 (157) |
| 13 | LTPD | ss8981611179 | Nov 02, 2024 (157) |
| 14 |
gnomAD v4 - Exomes
Submission ignored due to conflicting rows: |
- | Nov 02, 2024 (157) |
| 15 |
gnomAD v4 - Exomes
Submission ignored due to conflicting rows: |
- | Nov 02, 2024 (157) |
| 16 | ClinVar | RCV000014913.5 | Oct 11, 2018 (152) |
| 17 | ClinVar | RCV000114743.4 | Oct 11, 2018 (152) |
| 18 | ClinVar | RCV000419545.1 | Oct 11, 2018 (152) |
| 19 | ClinVar | RCV000419583.1 | Oct 11, 2018 (152) |
| 20 | ClinVar | RCV000424942.1 | Oct 11, 2018 (152) |
| 21 | ClinVar | RCV000426328.1 | Oct 11, 2018 (152) |
| 22 | ClinVar | RCV000427817.1 | Oct 11, 2018 (152) |
| 23 | ClinVar | RCV000428963.1 | Oct 11, 2018 (152) |
| 24 | ClinVar | RCV000434327.1 | Oct 11, 2018 (152) |
| 25 | ClinVar | RCV000436341.1 | Oct 11, 2018 (152) |
| 26 | ClinVar | RCV000437450.1 | Oct 11, 2018 (152) |
| 27 | ClinVar | RCV000438070.2 | Nov 02, 2024 (157) |
| 28 | ClinVar | RCV000444449.1 | Oct 11, 2018 (152) |
| 29 | ClinVar | RCV000445167.1 | Oct 11, 2018 (152) |
| 30 | ClinVar | RCV001781267.4 | Nov 02, 2024 (157) |
History tab displays RefSNPs (Associated ID) from previous builds (Build) that now support the current RefSNP, and the dates, when the history was updated for each Associated ID (History Updated).
| Submission IDs | Observation SPDI | Canonical SPDI | Source RSIDs |
|---|---|---|---|
| ss6403965963, ss8442107653, ss8935520788, ss8981611179 | NC_000001.10:115258744:C:A | NC_000001.11:114716123:C:A | (self) |
| RCV000445167.1, ss275515078, ss6408181591 | NC_000001.11:114716123:C:A | NC_000001.11:114716123:C:A | (self) |
| ss6403965963, ss8442107654, ss8799401649, ss8935520788 | NC_000001.10:115258744:C:G | NC_000001.11:114716123:C:G | (self) |
| RCV000014913.5, RCV000114743.4, RCV000419545.1, RCV000419583.1, RCV000424942.1, RCV000426328.1, RCV000427817.1, RCV000428963.1, RCV000434327.1, RCV000437450.1, RCV000438070.2, RCV000444449.1, RCV001781267.4, ss256302352, ss275515080, ss6408181592 | NC_000001.11:114716123:C:G | NC_000001.11:114716123:C:G | (self) |
| ss6403965963, ss8442107655, ss8935520788 | NC_000001.10:115258744:C:T | NC_000001.11:114716123:C:T | (self) |
| RCV000436341.1, ss275515081 | NC_000001.11:114716123:C:T | NC_000001.11:114716123:C:T | (self) |
Publications tab displays PubMed articles citing the variation as a listing of PMID, Title, Author, Year, Journal, ordered by Year, descending.
| PMID | Title | Author | Year | Journal |
|---|---|---|---|---|
| 2674680 | N-ras mutations in human cutaneous melanoma from sun-exposed body sites. | van 't Veer LJ et al. | 1989 | Molecular and cellular biology |
| 3102434 | Amino-acid substitution at codon 13 of the N-ras oncogene in rectal cancer in a Japanese patient. | Nitta N et al. | 1987 | Japanese journal of cancer research |
| 8120410 | Ras mutations in human melanoma: a marker of malignant progression. | Ball NJ et al. | 1994 | The Journal of investigative dermatology |
| 16291983 | Distinct sets of genetic alterations in melanoma. | Curtin JA et al. | 2005 | The New England journal of medicine |
| 18390968 | Phase I pharmacokinetic and pharmacodynamic study of the oral, small-molecule mitogen-activated protein kinase kinase 1/2 inhibitor AZD6244 (ARRY-142886) in patients with advanced cancers. | Adjei AA et al. | 2008 | Journal of clinical oncology |
| 18633438 | Genotypic and gene expression studies in congenital melanocytic nevi: insight into initial steps of melanotumorigenesis. | Dessars B et al. | 2009 | The Journal of investigative dermatology |
| 20130576 | RAF inhibitors prime wild-type RAF to activate the MAPK pathway and enhance growth. | Hatzivassiliou G et al. | 2010 | Nature |
| 20179705 | RAF inhibitors transactivate RAF dimers and ERK signalling in cells with wild-type BRAF. | Poulikakos PI et al. | 2010 | Nature |
| 22962325 | Intratumoral molecular heterogeneity in a BRAF-mutant, BRAF inhibitor-resistant melanoma: a case illustrating the challenges for personalized medicine. | Wilmott JS et al. | 2012 | Molecular cancer therapeutics |
| 23414587 | MEK162 for patients with advanced melanoma harbouring NRAS or Val600 BRAF mutations: a non-randomised, open-label phase 2 study. | Ascierto PA et al. | 2013 | The Lancet. Oncology |
| 25157968 | Prospective enterprise-level molecular genotyping of a cohort of cancer patients. | MacConaill LE et al. | 2014 | The Journal of molecular diagnostics |
| 26619011 | Identifying recurrent mutations in cancer reveals widespread lineage diversity and mutational specificity. | Chang MT et al. | 2016 | Nature biotechnology |
The Flanks tab provides retrieving flanking sequences of a SNP on all molecules that have placements.
Genomic regions, transcripts, and products
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Help
NCBI Graphical Sequence Viewer display of the genomic region, transcripts and protein products for the reported RefSNP (rs).
Use the zoom option to view the nucleotides around the RefSNP and find other neighboring RefSNPs.
Visit Sequence Viewer for help with navigating inside the display and modifying the selection of displayed data tracks.
NCBI Graphical Sequence Viewer display of the genomic region, transcripts and protein products for the reported RefSNP (rs).
Use the zoom option to view the nucleotides around the RefSNP and find other neighboring RefSNPs.
Visit Sequence Viewer for help with navigating inside the display and modifying the selection of displayed data tracks.