chr21:43094667:T>G Detail (hg38) (U2AF1)
Information
Genome
| Assembly | Position |
|---|---|
| hg19 | chr21:44,514,777-44,514,777 View the variant detail on this assembly version. |
| hg38 | chr21:43,094,667-43,094,667 |
HGVS
| Type | Transcript | Protein |
|---|---|---|
| RefSeq | NM_006758.2:c.470A>C | NP_006749.1:p.Gln157Pro |
| NM_001025203.1:c.470A>C | NP_001020374.1:p.Gln157Pro | |
| Ensemble | ENST00000291552.9:c.470A>C | ENST00000291552.9:p.Gln157Pro |
Summary
MGeND
| Clinical significance | |
| Variant entry | |
| GWAS entry | |
| Disease area statistics | Show details |
Frequency
| JP | HGVD:[No Data.] |
| ToMMo:[No Data.] | |
| NCBN:[No Data.] | |
| NCBN(Hondo):[No Data.] | |
| NCBN(Ryukyu):[No Data.] | |
| East asia | ExAC:<0.001 |
Prediction
ClinVar
| Clinical Significance |
Likely pathogenic
|
| Review star |  |
| Show details | |
Disease area statistics
[No Data.]
MGeND
[No Data.]
ClinVar
| Clinical significance | Last evaluated | Review status | Condition | Origin | Links |
|---|---|---|---|---|---|
|
Likely pathogenic
|
2016-03-10 | no assertion criteria provided | acute myeloid leukemia |
somatic
|
Detail |
not provided
|
2016-03-10 | no assertion provided | myelodysplastic syndrome |
somatic
|
Detail |
|
Likely pathogenic
|
2022-03-15 | criteria provided, single submitter | not provided |
germline
|
Detail |
CIViC
| Disease | Drug | EL | ET | ED | CS | VO | TR | Pubmed | Links |
|---|---|---|---|---|---|---|---|---|---|
| acute myeloid leukemia | B |
Diagnostic
|
Does Not Support
|
Positive | Somatic | 3 | 23029227 | Detail | |
| acute myeloid leukemia | B |
Prognostic
|
Does Not Support
|
N/A | Somatic | 2 | 23029227 | Detail | |
| myelodysplastic syndrome | B |
Prognostic
|
Does Not Support
|
N/A | Somatic | 2 | 23029227 | Detail | |
| myelodysplastic syndrome | B |
Prognostic
|
Supports
|
Poor Outcome | Somatic | 3 | 23861105 | Detail |
DisGeNET
| Score | Disease name | Description | Source | Pubmed | Links |
|---|---|---|---|---|---|
| <0.001 | de novo myelodysplastic syndromes | We previously identified missense mutations in the U2AF1 splicing factor affecti... | BeFree | 25311244 | Detail |
| <0.001 | Miller Dieker syndrome | We previously identified missense mutations in the U2AF1 splicing factor affecti... | BeFree | 25311244 | Detail |
| <0.001 | de novo myelodysplastic syndromes | We previously identified missense mutations in the U2AF1 splicing factor affecti... | BeFree | 25311244 | Detail |
Annotation
Annotations
| Descrption | Source | Links |
|---|---|---|
| Age, sex, FAB subtype and karyotypes were not statistically significant between AML patients with U2... | CIViC Evidence | Detail |
| In patients with AML, those who harbor Q157P/R mutation of U2AF1 do not show a statistically signifi... | CIViC Evidence | Detail |
| In patients with MDS, those who harbor Q157P/R mutation of U2AF do not show statistical significance... | CIViC Evidence | Detail |
| After adjusting for age and cancer stage, presence of U2AF mutation such as Q157P/R is prognostic fo... | CIViC Evidence | Detail |
| NM_006758.3(U2AF1):c.470A>C (p.Gln157Pro) AND Acute myeloid leukemia | ClinVar | Detail |
| NM_006758.3(U2AF1):c.470A>C (p.Gln157Pro) AND Myelodysplastic syndrome | ClinVar | Detail |
| NM_006758.3(U2AF1):c.470A>C (p.Gln157Pro) AND not provided | ClinVar | Detail |
| We previously identified missense mutations in the U2AF1 splicing factor affecting codons S34 (S34F ... | DisGeNET | Detail |
| We previously identified missense mutations in the U2AF1 splicing factor affecting codons S34 (S34F ... | DisGeNET | Detail |
| We previously identified missense mutations in the U2AF1 splicing factor affecting codons S34 (S34F ... | DisGeNET | Detail |
Overlapped Transcript Coordinates
| Gene | Transcript ID | Exon Number | Chromosome | Start | Stop | Type | Amino Mutation | Transcript Position | Links |
|---|
Overlapped Transcript
| Gene | Transcript ID | Chromosome | Start | Stop | Links |
|---|
- Gene
- -
- dbSNP
- rs371246226 dbSNP
- Genome
- hg38
- Position
- chr21:43,094,667-43,094,667
- Variant Type
- snv
- Reference Allele
- T
- Alternative Allele
- G
- East Asian Chromosome Counts (ExAC)
- 8634
- East Asian Allele Counts (ExAC)
- 1
- East Asian Heterozygous Counts (ExAC)
- 1
- East Asian Homozygous Counts (ExAC)
- 0
- East Asian Allele Frequency (ExAC)
- 1.1582117211026175E-4
- Chromosome Counts in All Race (ExAC)
- 121008
- Allele Counts in All Race (ExAC)
- 4
- Heterozygous Counts in All Race (ExAC)
- 4
- Homozygous Counts in All Race (ExAC)
- 0
- Allele Frequency in All Race (ExAC)
- 3.305566574110803E-5
- Variant (CIViC) (CIViC Variant)
- Q157P/R
- Transcript 1 (CIViC Variant)
- ENST00000291552.4
- Variant URL (CIViC Variant)
- https://civic.genome.wustl.edu/links/variants/127
- Summary (CIViC Variant)
- U2AF1 Q157P/R has been shown to be a recurrent mutation in acute myeloid leukemia (AML), myelodysplastic syndromes (MDS) and lung adenocarcinomas. This mutation is less common than the S34F mutation, occurs in the second zinc finger domain of U2AF1 and has been demonstrated to alter splicing. The impact of U2AF1 mutations on overall survival in MDS has been debated, however, patients with U2AF1 mutations were shown to be at an increased risk of transformation to secondary AML. The presence of this mutation was not associated with a specific prognostic outcome in AML when compared to U2AF1 wildtype patients.
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