PharmGKB clinical annotations provide information about variant-drug pairs based on a summary of the individual variant annotations in the database. Therefore, each clinical annotation could represent information from a single paper or multiple papers. The rating system used to assign "Strength of Evidence" levels is described here. The individual variant annotations, including the PMID for each supporting PubMed publication, can be found on the "PGx Research" tab above.
This information is manually curated by PharmGKB. All alleles are displayed on the positive chromosomal strand.
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PharmGKB variant annotations provide information about variant-drug pairs or variant-disease pairs based on individual PubMed publications. Each annotation represents information from a single paper and the goal is to report the information that the author states, not an interpretation of the paper. The PMID for supporting PubMed publications is found in the "Evidence" field.
Information presented, including study size, allele frequencies and statistics is taken directly from the publication. However, if the author does not correct p-values in cases of multiple hypotheses, curators may apply a Bonferroni correction. Curators attempt to report study size based on the actual number of participants used for the calculation of the association statistics, so the number may vary slightly from what is reported in the abstract of the paper. OMB Race Category information is derived from the paper and mapped to standardized categories. Category definitions may be found by clicking on the "OMB Race Category" link.
List of all variant annotations for this variant.
There are 32 annotations for this variant. Register or sign in to see them.
| PharmGKB Accession ID: | PA166154070 |
| Type: | SNP |
| Class: | Stop Codon |
| Clinical Significance: | Not reported |
| Genes: | CYP2C19 |
rs4986893 (c.636G>A) is the defining polymorphism of the CYP2C19*3 allele (previously referred to as CYP2C19m2) and is a G>A transition in exon 4 that results in a premature termination codon at amino acid 212 (p.W212X) [Article:7969038]. The CYP2C19*3 allele frequencies in most populations is below 1%; however, it is more prevalent among Asians (2-9%) [Article:21716271] For more information see also CYP2C19*3 haplotype page.
| Citation |
PharmGKB summary: very important pharmacogene information for cytochrome P450, family 2, subfamily C, polypeptide 19. Pharmacogenetics and genomics. 2011. Scott Stuart A, Sangkuhl Katrin, Shuldiner Alan R, Hulot Jean-Sébastien, Thorn Caroline F, Altman Russ B, Klein Teri E.
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|---|---|
| Reviewed | 09/12/2011 |
| Key Publications: |
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| Drugs / Other Molecules |
Drug (25)
amitriptyline
carisoprodol
citalopram
clomipramine
cyclophosphamide
hexobarbital
imipramine
indomethacin
lansoprazole
mephenytoin
methylphenobarbital
moclobemide
nelfinavir
nilutamide
omeprazole
pantoprazole
phenobarbital
phenytoin
primidone
progesterone
proguanil
propranolol
rabeprazole
teniposide
warfarin
|
Name: CYP2C19:636G>A
mRNA Variant & GenBank ID: G>A at 636 on NM_000769
Genomic Variant & GenBank ID: G>A at 19952 on AY796203.1
Protein Variant & GenBank ID: Trp>Ter at 212 on NP_000760
Key Haplotypes CYP2C19*3
| Evidence | Drug |
|---|---|
| mephenytoin |
| Evidence | Disease |
|---|
| Evidence | Publication |
|---|---|
| Differences in the incidence of the CYP2C19 polymorphism affecting the S-mephenytoin phenotype in Chinese Han and Bai populations and identification of a new rare CYP2C19 mutant allele. The Journal of pharmacology and experimental therapeutics. 1997. Xiao Z S, et al.
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| Genotyping of S-mephenytoin 4'-hydroxylation in an extended Japanese population. Clinical pharmacology and therapeutics. 1996. Kubota T, et al.
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| Identification of a new genetic defect responsible for the polymorphism of (S)-mephenytoin metabolism in Japanese. Molecular pharmacology. 1994. De Morais S M, et al.
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