Allele Count: | 1 |
---|---|
Allele Number: | 5984 |
Allele Frequency: | 1.6711e-4 |
Number of Homozygotes: | 0 |
Dataset | Population | Population abbr | Allele Frequency |
---|---|---|---|
1KGP3 | East Asian | EAS | - |
South Asian | SAS | - | |
African | AFR | - | |
Americas | AMR | - | |
European ancestry | EUR | - | |
total | - | ||
gnomAD v3 Genomes | East Asian | EAS | 0.0 |
South Asian | SAS | 0.0 | |
Afican | AFR | 7.1874e-5 | |
Latino | AMR | 7.3475e-5 | |
Amish | AMI | 0.0 | |
European(Finnish) | FIN | 0.0 | |
European(non-Finnish) | NFE | 1.5530e-5 | |
Ashkenazi Jewish | ASJ | 0.0 | |
other | OTH | 0.0 | |
total | 3.5030e-5 |
Region | Gene ID | Gene Detail | Exonic function | Consequence | |
---|---|---|---|---|---|
Ensembl | exonic | CYP2D6 | - | nonsynonymous SNV | CYP2D6:ENST00000359033.4:exon6:c.C985T:p.R329C,CYP2D6:ENST00000389970.7:exon8:c.C1129T:p.R377C |
RefSeq | exonic | CYP2D6;CYP2D7 | - | nonsynonymous SNV | CYP2D6:NM_001025161:exon6:c.C985T:p.R329C,CYP2D6:NM_000106:exon7:c.C1138T:p.R380C |
Method | Score | Rank Score | predicted consequence |
---|---|---|---|
SIFT | 0.103 | 0.318 | T |
PolyPhen2_HDIV | 0.369 | 0.330 | B |
PolyPhen2_HVAR | 0.11 | 0.341 | B |
FATHMM | -1.33 | 0.799 | T |
CADD | 3.840 | 0.518 | 23.4 |
ClinVar Significance | ClinVar Disease Name | ClinVar Allele ID | Tag-value |
---|---|---|---|
- | - | - | - |
Loss of Function (LoF) variants are indentified by package LOFTEE developed recently by gnomAD group to assess stop-gained, splice site disrupting and frameshift variants as “low-confidence” (LC) or “high-confidence” (HC) LoF variants.
LoF | LoF_filter | LoF_flags | LoF_info |
---|---|---|---|
- | - | - | - |
Belong to Haplotype | Drug | Guideine | URL | CPIC_Level | PharmGKB_Level _of_Evidence | PGx_on_FDA _Label | CPIC_Publications_PMID |
---|---|---|---|---|---|---|---|
- | - | - | - | - | - | - | - |