Abstract
Pharmacokinetic variability is a major source of differences in drug response and can be due to genetic variants and/or drug-drug interactions. Cytochromes P450 are among the most studied enzymes from a pharmacokinetic point of view. Their activity can be measured by phenotyping, and/or predicted by genotyping. Depending on the presence of drugs and/or diseases that can affect their in vivo activity, both approaches can be complementary. In 2014, the Geneva cocktail using dried blood spots was validated in healthy volunteers for CYP450 phenotyping. Since its clinical implementation, it has been used in approximately 500 patients in various clinical situations. Our study aims to report the concordance between CYP450 genotype and phenotype in real-life patients. The prospectively collected data from patients who were genotyped and/or phenotyped between January 2014 and December 2020 were reviewed. A total of 537 patients were genotyped and/or phenotyped for CYP450 during this period, and 241 underwent simultaneous genotyping and phenotyping allowing for genotype/phenotype concordance assessment. Genotyping correctly predicted poor metabolizer phenotypes for most CYPs isoenzymes studied, whereas agreement was more variable for intermediate, normal, and ultrarapid metabolizers. Discrepancies between the phenotype predicted on the basis of genotyping and the measured phenotype were not always explained by concurrent medication (phenotypic switch). Therefore genotyping and phenotyping tests are complementary approaches when aiming to individualize drug therapy. In the 537 patients, the majority of clinical situations were observed with analgesic/anesthetic drugs (n = 187), followed by antidepressants (n = 153), antineoplastics (n = 97), and immunosuppressants (n = 93). Inefficacy (or low drug levels) and adverse drug reaction (or high drug levels) were the main reasons for testing. Genotype and/or phenotype results explained or at least contributed to the clinical event in 44% of cases.
Highlights
Patients vary in their response to drugs
Our study aims to report the concordance between Cytochromes P450 (CYP450) genotype and phenotype using the Geneva micrococktail in real-life patients
We evaluated in- and outpatients with CYP450 genotyping and/or phenotyping tests since 2014, the year of implementation of the Geneva micrococktail as used in its current formulation
Summary
Patients vary in their response to drugs. A dose that is effective in a given patient may cause an adverse drug reaction (ADR) in another patient or be ineffective. Several causes of variability can be cited, genetic- or disease-related changes in drug concentrations or responsiveness, poor compliance, drugdrug interactions (DDI). Variability in drug response can affect pharmacokinetics, pharmacodynamics, or both (Roden et al, 2019). Pharmacokinetic variability is a major source of differences in drug response and can be due to genetic variants, diseases themselves and/or DDI. Cytochromes P450 (CYP450) are among the most studied enzymes from a pharmacokinetic point of view. Their activity can be predicted by genotyping and/or measured by phenotyping
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