Impact of age, sex and cytochrome P450 genotype on quetiapine and N‐desalkylquetiapine serum concentrations: A study based on real‐world data from 8118 patients

Author:

Solhaug Vigdis1ORCID,Tveito Marit1,Waade Ragnhild Birkeland1ORCID,Høiseth Gudrun123,Molden Espen14ORCID,Smith Robert Løvsletten15ORCID

Affiliation:

1. Center for Psychopharmacology Diakonhjemmet Hospital Oslo Norway

2. Department of Forensic Sciences Oslo University Hospital Oslo Norway

3. Institute of Clinical Medicine University of Oslo Oslo Norway

4. Department of Pharmacy University of Oslo Oslo Norway

5. NORMENT Center, Institute of Clinical Medicine University of Oslo and Oslo University Hospital Oslo Norway

Abstract

AimsTo investigate the effect of aging, sex and cytochrome P450 (CYP) genotypes on the exposure of quetiapine (QUE) and the pharmacologically active metabolite N‐desalkylquetiapine (NDQ).MethodsPatients with serum concentrations of QUE and NDQ were included retrospectively from a therapeutic drug monitoring service. The outcome measures were concentration:dose (C:D) ratios of QUE and NDQ, and NDQ:QUE metabolic ratio. Linear mixed model analyses were used to evaluate the effects of age, sex and, subsequently, CYP2D6/3A genotypes.ResultsThe average age of the included population (n = 8118 patients) was 44 years (13.5% ≥65 years). The C:D ratio of QUE and NDQ gradually increased in patients aged >50 years compared to those aged 18–30 years, with 28 and 29% increase, respectively, for patients aged >70 years (P < .001). Compared to males, females had 15% lower QUE C:D ratio and 10% higher C:D ratio of NDQ (both P < .001). The NDQ:QUE metabolic ratio was 30% higher in females than in males (P < .001). For females ≥65 years, the NDQ C:D ratio was 36% higher compared to males <65 years (P < .001). A significantly higher NDQ C:D ratio was observed for CYP2D6 intermediate (+7%, P = .012) and poor (+17%, P = .001) compared to normal metabolizers. No effects of CYP3A4*22 and CYP3A5*1 allele variants were observed.ConclusionThis study shows an increase of the QUE and NDQ exposures during aging. Old age, female sex and CYP2D6 allele variants encoding reduced activity are factors associated with high NDQ exposure. Therefore, females ≥65 years carrying CYP2D6 allele variants encoding reduced activity have the highest risk of dose‐dependent side effects of NDQ during QUE treatment.

Publisher

Wiley

Subject

Pharmacology (medical),Pharmacology

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