Dutch Pharmacogenetics Working Group (DPWG) guideline for the gene-drug interaction between CYP2C19 and CYP2D6 and SSRIs

Jurriaan M J L Brouwer; Marga Nijenhuis; Bianca Soree; Henk-Jan Guchelaar; Jesse J Swen; Ron H N van Schaik; Jan van der Weide; Gerard A P J M Rongen; Anne-Marie Buunk; Nienke J de Boer-Veger; Elisa J F Houwink; Roos van Westrhenen; Bob Wilffert; Vera H M Deneer; Hans Mulder

doi:10.1038/s41431-021-01004-7

. 2021 Nov 16;30(10):1114–1120. doi: 10.1038/s41431-021-01004-7

Dutch Pharmacogenetics Working Group (DPWG) guideline for the gene-drug interaction between CYP2C19 and CYP2D6 and SSRIs

Jurriaan M J L Brouwer ^1,^2,³, Marga Nijenhuis ^4,^✉, Bianca Soree ⁴, Henk-Jan Guchelaar ⁵, Jesse J Swen ⁵, Ron H N van Schaik ⁶, Jan van der Weide ⁷, Gerard A P J M Rongen ^8,⁹, Anne-Marie Buunk ¹⁰, Nienke J de Boer-Veger ¹¹, Elisa J F Houwink ^12,¹³, Roos van Westrhenen ^14,^15,¹⁶, Bob Wilffert ^17,¹⁸, Vera H M Deneer ^19,²⁰, Hans Mulder ¹

¹Department of Clinical Pharmacy, Wilhelmina Hospital Assen, Assen, The Netherlands

²GGZ Drenthe Mental Health Services Drenthe, Assen, The Netherlands

³Department of Psychiatry, Research School of Behavioural and Cognitive Neurosciences, University of Groningen, University Medical Centre Groningen, Groningen, The Netherlands

⁴Royal Dutch Pharmacists Association (KNMP), The Hague, The Netherlands

⁵Department of Clinical Pharmacy & Toxicology, Leiden University Medical Centre, Leiden, The Netherlands

⁶Department of Clinical Chemistry, Erasmus University Medical Centre, Rotterdam, The Netherlands

⁷Department of Clinical Chemistry, St. Jansdal Hospital, Harderwijk, The Netherlands

⁸Department of Internal Medicine, Radboud University Medical Centre, Nijmegen, The Netherlands

⁹Department of Pharmacology and Toxicology, Radboud University Medical Centre, Nijmegen, The Netherlands

¹⁰Pharmacy De Katwijkse Apotheek, Katwijk, The Netherlands

¹¹Pharmacy Boterdiep, Groningen, The Netherlands

¹²Department of Public Health and Primary Care (PHEG), Leiden University Medical Centre, Leiden, The Netherlands

¹³National eHealth Living Lab (NELL), Leiden, The Netherlands

¹⁴Parnassia Psychiatric Institute/PsyQ, Amsterdam, The Netherlands

¹⁵Department of Psychiatry and Neuropsychology, Maastricht University, Maastricht, The Netherlands

¹⁶Institute of Psychiatry, Psychology and Neuroscience (IoPPN), King’s College London, London, United Kingdom

¹⁷Department of Clinical Pharmacy & Pharmacology, University of Groningen, University Medical Centre Groningen, Groningen, The Netherlands

¹⁸Department of PharmacoTherapy, -Epidemiology & -Economics, Groningen Research Institute of Pharmacy, University of Groningen, Groningen, The Netherlands

¹⁹Department of Clinical Pharmacy, Division Laboratories, Pharmacy and Biomedical Genetics, University Medical Centre Utrecht, Utrecht, The Netherlands

²⁰Department of Pharmaceutical Sciences, Division of Pharmacoepidemiology and Clinical Pharmacology, Utrecht Institute for Pharmaceutical Sciences (UIPS), Utrecht University, Utrecht, The Netherlands

^✉

Corresponding author.

PMCID: PMC9553948 PMID: 34782755

Abstract

The Dutch Pharmacogenetics Working Group (DPWG) guideline presented here, presents the gene-drug interaction between the genes CYP2C19 and CYP2D6 and antidepressants of the selective serotonin reuptake inhibitor type (SSRIs). Both genes’ genotypes are translated into predicted normal metabolizer (NM), intermediate metabolizer (IM), poor metabolizer (PM), or ultra-rapid metabolizer (UM). Evidence-based dose recommendations were obtained, based on a structured analysis of published literature. In CYP2C19 PM patients, escitalopram dose should not exceed 50% of the normal maximum dose. In CYP2C19 IM patients, this is 75% of the normal maximum dose. Escitalopram should be avoided in UM patients. In CYP2C19 PM patients, citalopram dose should not exceed 50% of the normal maximum dose. In CYP2C19 IM patients, this is 70% (65–75%) of the normal maximum dose. In contrast to escitalopram, no action is needed for CYP2C19 UM patients. In CYP2C19 PM patients, sertraline dose should not exceed 37.5% of the normal maximum dose. No action is needed for CYP2C19 IM and UM patients. In CYP2D6 UM patients, paroxetine should be avoided. No action is needed for CYP2D6 PM and IM patients. In addition, no action is needed for the other gene-drug combinations. Clinical effects (increase in adverse events or decrease in efficacy) were lacking for these other gene-drug combinations. DPWG classifies CYP2C19 genotyping before the start of escitalopram, citalopram, and sertraline, and CYP2D6 genotyping before the start of paroxetine as “potentially beneficial” for toxicity/effectivity predictions. This indicates that genotyping prior to treatment can be considered on an individual patient basis.

Subject terms: Genetics, Psychology

Introduction

Pharmacogenomics (PGx) encompasses the notion that genetic variation can lead to variation in drug response. This shifts “one-size fits all” pharmacotherapy towards “tailor-made” pharmacotherapy. Although PGx is widely acknowledged, its implementation in daily clinical practice remains challenging [1]. One of the barriers preventing implementation in daily clinical practice was the lack of clear guidelines on how to interpret and apply PGx test results. To resolve this barrier, the Royal Dutch Pharmacists Association (KNMP) established the Dutch Pharmacogenetics Working Group (DPWG) in 2005 [2]. The main objectives of the DPWG are (1) to develop PGx informed therapeutic recommendations based on systematic literature review, and (2) to assist physicians and pharmacists by integrating the recommendations into computerized systems for drug prescription, dispensing, and automated medication surveillance. The DPWG is a multidisciplinary group in which (clinical) pharmacists, physicians, clinical pharmacologists, clinical chemists and epidemiologists are represented. Recently, the DPWG guidelines were endorsed by the European Association of Clinical Pharmacology and Therapeutics and the European Association of Hospital Pharmacists. The DPWG guidelines and future updates will be published in the European Journal of Human Genetics, in order to meet the public request for this information also outside the Dutch health care system.

This guideline presents the gene-drug interaction between CYP2D6 and CYP2C19 and antidepressants of the selective serotonin reuptake inhibitor type (SSRIs). First, it describes background information regarding genetic variation in the genes CYP2D6 and CYP2C19. Second, the evidence for gene-drug interactions between CYP2D6 and CYP2C19 and individual SSRIs is presented (Supplementary Tables 1–9), as is the clinical implication score for these gene-drug interactions (Implications for clinical practice section). Finally recommendations are compared to the Clinical Pharmacogenetics Implementation Consortium (CPIC) guidelines [3].

Drugs: selective serotonin reuptake inhibitors

SSRIs are licensed for several indications, such as the treatment of depression, anxiety disorders, and obsessive-compulsive disorders. The mechanism of action of SSRIs mostly relies on the inhibition of reuptake of serotonin by the serotonin transporter (SERT). This is thought to be responsible for the antidepressant effect. However, treatment response and remission is only present in one third of the patients [4], while in addition antidepressant drugs may also lead to side effects, such as agitation, headache, gastro-intestinal symptoms as vomiting or diarrhoea, and (rarely) serotonergic syndrome. Selection of an appropriate antidepressant drug is, to a great extent, still empirical based [5]. Whether there is sufficient effect or presence of side effects, relies among others on the metabolism of the SSRI by the Cytochrome P450 system.

Citalopram is a racemic mixture of S- and R-citalopram, whereby escitalopram (the S-enantiomer) is the active enantiomer. Citalopram and escitalopram are primarily metabolized by CYP2C19 and to a lesser extent by CYP3A4 to an inactive metabolite.

Fluoxetine is metabolized extensively to the active and equipotent metabolite norfluoxetine by CYP2D6. CYP2C9, CYP2C19, and CYP3A4 are, possibly, also involved. Fluoxetine and norfluoxetine are potent inhibitors of CYP2D6, moderate inhibitors of CYP2C9, and mild to moderate inhibitors of CYP2C19 and CYP3A4.

Paroxetine is a potent antagonist of SERT and is metabolized by CYP2D6 and CYP3A4 to inactive metabolites. In addition, it is a potent inhibitor of CYP2D6.

Fluvoxamine is converted by CYP2D6 and to a lesser extent by CYP1A2. Fluvoxamine is a strong inhibitor of CYP1A2, a moderate inhibitor of CYP2C19 and CYP3A4, and a weak inhibitor of CYP2D6.

Sertraline is metabolized to N-desmethylsertraline by CYP2C19, CYP2B6, and to a far lesser extent by CYP2C9, CYP3A4, and CYP2D6. Sertraline does not significantly inhibit CYP enzymes.

Gene: CYP2C19 (Cytochrome P450 family 2 subfamily C member 19)

CYP2C19, formulated as Cytochrome P450 family 2 subfamily C member 19, is located on chromosome 10q23.33, has 9 exons, and a total size of approximately 120 kb. It encodes the metabolic enzyme CYP2C19 and is expressed in the liver, duodenum, small intestine, stomach and gall bladder [6]. With over 30 different allele variants in CYP2C19 being identified and described in the literature [7–9], each allele variant is indicated with an asterisk and a number, with *1 being the wild type allele. Except for *2, *3 and *17, the prevalence of individual variants is low. The *2- and *3-alleles are null alleles, leading to an inactive CYP2C19 enzyme. In contrast, the *17-allele results in an increased CYP2C19 enzyme activity. Supplementary Table 10A lists the most important allele variants and their predicted effect on the enzyme activity of the CYP2C19 enzyme (including rs-numbers and HGVS nomenclature).

The frequency of the various CYP2C19 variant alleles and the associated phenotypes varies significantly between nations and ethnic groups [10]. The *2-allele has a frequency of ~15% in White and African populations, while in Asian populations the frequency is ~30%. The *3-allele has a very low frequency in White and African populations and a frequency of 5–11% in Asian populations. As a result, 12–23% in Asian populations as well as 1–7.5% in White and African populations have a complete CYP2C19 deficiency (CYP2C19 poor metabolizers (PM)). In contrast, the frequency of the *17-allele is 18–27% in White and African populations and 1–4% in Asian populations [10–12], resulting in a percentage of 3–7% in White and African populations and 0–0.2% in Asian populations being CYP2C19*17 homozygotes (ultra-rapid metabolizers (UM)). Supplementary Table 10B provides an overview of the frequencies of the alleles most important for genotyping in different populations.

Translation of genotype to predicted phenotype

The DPWG defines patients with one allele leading to a CYP2C19 enzyme with diminished or no activity as CYP2C19 intermediate metabolizers (IM), and patients homozygous or compound heterozygous for such alleles as CYP2C19 PMs. The CYP2C19 IM phenotype includes patients compound heterozygous for a *17-allele and an allele leading to a CYP2C19 enzyme with no or diminished activity, because the effect of the *17-allele on enzyme activity has been shown to be small and not to compensate for the effect of a null allele. For the same reason, the DPWG decided to include the *1/*17 genotype in the CYP2C19 normal metabolizer (NM) phenotype (see Supplementary Material 1A for a detailed rationale). Therefore, the DPWG only assigns *17/*17 to a separate genotype, i.e., CYP2C19 UM.

The genotype to predicted phenotype translation is summarized in Table 1. A complete genotype to predicted phenotype translation table, which can be used to programme the translation of genotype results into predicted phenotypes in laboratory information systems, can be found in Supplementary Table 11.

Table 1.

Translation of genotype to predicted phenotype for CYP2C19 and CYP2D6.

Gene	Examples of diplotypes	Genotypes	Predicted phenotypes
CYP2C19	1/1, 1/17	Two normal function alleles or one normal function and one increased function allele.	Normal metabolizer
	1/2, 1/3, 2/17, 3/17	One no or decreased function allele in combination with either one normal function allele or one increased function allele.	Intermediate metabolizer
	2/2, 2/3, 3/3	Two no or decreased function alleles.	Poor metabolizer
	17/17	Two increased function alleles.	Ultrarapid metabolizer
CYP2D6	1/1, 1/41, 1/41×3^a	Gene dose^b 1.5–2.5	Normal metabolizer
	1/4, 41/41, 4/41	Gene dose^b 0.5–1	Intermediate metabolizer
	4/4, 4/5	Gene dose^b 0	Poor metabolizer
	1/1×2, 1/2×2, 2×3/4, 1/41×4^a	Gene dose^b ≥ 3	Ultrarapid metabolizer

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The *-alleles mentioned in the table above are characterized by the following sequence variations:

CYP2C19*1: defined as the allele without variations affecting enzyme activity (in clinical practice as the allele without any of the determined variations).

CYP2C19*2: rs-number: rs12769205 and rs4244285; NC_000010.11(NM_000769.2): c.[332-23 A > G; 681 G > A]; NC_000010.11: g.[94775367 A > G; 94781859 G > A].

CYP2C19*3: rs-number: rs4986893; NM_000769.2: c.636 G > A; NP_000760.1: p.(Trp212*); NC_000010.11: g.94780653 G > A.

CYP2C19*17: rs-number: rs12248560; NM_000769.2 c.−806C > T; NP_000760.1: p.(Ile331Val); NC_000010.11: g.94761900 C > T.

CYP2D6*1: defined as the allele without variations affecting enzyme activity (in clinical practice as the allele without any of the determined variations).

CYP2D6*2: rs-numbers: rs16947 and rs1135840; NM_000106.6: c.[886 C > T; 1457 G > C]; NP_000097.3: p.(Arg296Cys; Ser486Thr); NC_000022.11: g.[42127941 G > A; 42126611 C > G].

CYP2D6*4: rs-number: rs3892097; NG_008376.3(NM_000106.6): c.506-1 G > A; protein sequence not available; NC_000022.11: g.42128945 C > T.

CYP2D6*5: CYP2D6 full gene deletion.

CYP2D6*41: rs-numbers: rs16947, rs28371725 and rs1135840; NG_008376.3(NM_000106.6): c.[886 C > T; 985 + 39 G > A; 1457 G > C]; NP_000097.3: p.(Arg296Cys; protein sequence not available; Ser486Thr); NC_000022.11: g.[42127941 G > A; 42127803 C > T; 42126611 C > G].

^ax2 denotes a gene duplication, x3 a gene triplication and x4 a gene quadruplication.

^bThe gene dose is 1 for an allele encoding a fully functional enzyme, 0.5 for an allele encoding a reduced activity enzyme and 0 for an allele encoding an inactive enzyme.

Gene: CYP2D6 (Cytochrome P450 family 2 subfamily D member 6)

For CYP2D6, a detailed explanation of the gene and its variants can be found in Supplementary Materials 1B as CYP2D6 has previously been described elsewhere as part of the DPWG guidelines [13]. In addition, a list of the most important allele variants and their effect on the enzyme activity of the CYP2D6 enzyme (including rs-numbers and HGVS nomenclature) can be found in Supplementary Table 12A, whereas Supplementary Table 12B provides an overview of the frequencies of the alleles most important for genotyping in different populations. The genotype to predicted phenotype translation is summarized in Table 1. A complete genotype to predicted phenotype translation table, which can be used to programme the translation of genotype results into predicted phenotypes in laboratory information systems, can be found in Supplementary Table 13.

Gene-drug interaction

Pharmacological mechanism

CYP2D6 and CYP2C19 are major metabolizing enzymes for SSRIs. Increased enzyme activity of CYP2C19 is expected to lower plasma concentrations of escitalopram, citalopram, and sertraline, therefore potentially hampering the antidepressant effect. On the other hand, decreased enzyme activity of CYP2C19 is associated with increased plasma concentrations of escitalopram, citalopram, and sertraline. The increased plasma concentrations may result in SSRI-induced side effects.

Increased enzyme activity of CYP2D6 is expected to lower plasma concentrations of paroxetine, fluoxetine, and fluvoxamine, therefore potentially decreasing the antidepressant effect. On the other hand, decreased enzyme activity of CYP2D6 is associated with increased plasma concentrations of paroxetine, fluoxetine, and fluvoxamine. The increased plasma concentrations may result in SSRI-induced side effects. However, as the therapeutic ranges of SSRIs are relatively broad and the preferred 70% SERT occupancy, which should be achieved for optimal clinical outcome, seems to occur at relatively low doses [14, 15], changes in plasma concentrations might not have clinical consequences.

For paroxetine and fluoxetine specifically, differences in clinical effect and/or prevalence of side effects between CYP2D6 genotypes is expected to be relatively small. This is because of the strong inhibitory effect of these drugs on CYP2D6, in which phenotypes change from NM to PM during chronic dosing [16, 17].

Supporting body of evidence

A detailed description of the methods used for literature collection, assessment and preparation of the gene-drug monograph has previously been published elsewhere [2, 18]. In brief, a systematic review of literature was performed, relevant articles were summarized, and therapeutic recommendations were proposed by a scientist of the Royal Dutch Pharmacists Association (predominantly MN from 2007). The performed search and selection strategy can be found in Supplementary Material 1C. Each article was provided with two scores: (1) the level of evidence and (2) the clinical impact. The level of evidence was scored using a five-point scale ranging from 0 to 4, with 0 being the lowest (data on file) and 4 being the highest (published controlled studies of good quality or meta-analyses). The impact of the clinical effect was scored using a seven-point scale ranging from AA^# to F, with AA^# indicating a positive effect and F indicating the highest negative effect. The criteria used to develop these scores have been published in detail previously [2, 18]. The clinical impact scale runs parallel to the Common Terminology Criteria for Adverse Events (CTCAE), with CTCAE grade 5 severity being equal to the clinical relevance score F (death) and CTCAE grade 1 severity being equal to the clinical relevance score B. Clinical relevance scores AA^#, AA and A are defined as a positive clinical effect, no kinetic or clinical effect, and a kinetic effect or not clinically relevant effect, respectively, as these do not exist in the CTCAE.

The summaries and scores of the articles reviewed to devise this guideline can be found in the Supplementary Table 1 through 9. The summary and scores of each article were checked by two independent DPWG members. The DPWG made the final decision on the therapeutic recommendations.

General conclusions of evidence

Detailed rationales for the conclusions of evidence and the kinetic and clinical consequences for each predicted phenotype are provided in Supplementary Table 14 through 22. A brief description is given below.

CYP2C19 – Escitalopram

A study showed an increase in therapy failure for PM and UM (increase in the percentage of patients switched to another antidepressant). For this reason, the DPWG decided to recommend therapy adjustment for UM.

As IM and PM lead to a distinct increase in escitalopram plasma concentration and so in the risk of escitalopram-induced QT prolongation, a decision was made to recommend to lower the maximum dose in IM and PM patients to compensate for this plasma concentration increase. Details are provided in Supplementary Table 14, the summaries of reviewed articles in Supplementary Table 1.

CYP2C19 – Citalopram

As a study found a positive correlation between QT_c interval and dose, it was decided to recommend to lower the maximum dose in IM and PM patients to compensate for the plasma concentration increase in these patients. For UM, no warning is issued for the gene-drug interaction, as there were no significant clinical effects reported. Details are provided in Supplementary Table 15, the summaries of reviewed articles in Supplementary Table 2.

CYP2C19 – Sertraline

For sertraline, the CYP2C19 phenotype was shown to affect sertraline exposure, but no clinical consequences were reported. The DPWG recommends a decrease in the maximum dose for PM patients, due to the relative high increase in concentration compared to the therapeutic range. Because of the smaller effect in IM and UM patients, the DPWG decided that there was not enough evidence to recommend an adjustment of therapy for these patients. Details are provided in Supplementary Table 16, the summaries of reviewed articles in Supplementary Table 3.

CYP2D6 – Paroxetine

For most CYP2D6 UM patients, the plasma concentration at steady state was below the detection limit and therapeutic efficacy was lacking. As a precaution, the DPWG recommends selecting an alternative. As no clinical effects were reported for IM and PM, no action is required for these gene-drug interactions. Details are provided in Supplementary Table 17, the summaries of reviewed articles in Supplementary Table 4.

CYP2D6 – Fluoxetine

Studies found an effect of CYP2D6 phenotype on the conversion of fluoxetine to its active metabolite, but no effect on the sum of the plasma concentrations of the active substances, response and side effects. Thus, no adjustment of therapy is needed for these gene-drug interactions. Details are provided in Supplementary Table 18, the summaries of reviewed articles in Supplementary Table 5.

CYP2D6 – Fluvoxamine

Studies found a not very strong effect of the CYP2D6 phenotype on fluvoxamine exposure and no effect on response and side effect. For this reason, the DPWG decided that no adjustment of therapy is needed for these gene-drug interactions. Details are provided in Supplementary Table 19, the summaries of reviewed articles in Supplementary Table 6.

CYP2C19 – Fluvoxamine, CYP2D6 – Escitalopram/citalopram, and CYP2D6 – Sertraline

No gene-drug interactions are expected for these three gene-drug combinations. Indeed, the systematic reviews confirmed that there is no or insufficient evidence to support a gene-drug interaction for these three combinations. This confirms the suitability of these drugs as possible alternatives for other SSRIs in patients with a CYP2C19 or CYP2D6 variant, respectively. Details are provided in Supplementary Table 20 through 22, the summaries of reviewed articles in Supplementary Table 7 through 9.

Pharmacotherapeutic recommendations

The DPWG recommendations for therapy with SSRIs in patients known to have an aberrant CYP2C19 or CYP2D6 metabolizer status is summarized in Table 2. A more detailed version of the recommendations, including their rationale, is provided in Supplementary Tables 14 through 22. A brief version is indicated below.

Table 2.

Summary therapeutic recommendations based on CYP2C19 and CYP2D6 phenotype for escitalopram, citalopram, sertraline, paroxetine, fluoxetine, and fluvoxamine.

Drug	Gene	Phenotype	Therapeutic recommendation (if present)^a
Escitalopram	CYP2C19	PM	Do not exceed the following doses (50% of the standard maximum dose): - Adults up to 65 years: 10 mg/day - Adults 65 years or older: 5 mg/day
		IM	Do not exceed the following doses (75% of the standard maximum dose): - Adults <65 years: 15 mg/day - Adults 65 years or older: 7.5 mg/day
		UM	Avoid escitalopram. Antidepressants that are not metabolized or that are metabolized to a lesser extent by CYP2C19 are, for example, paroxetine or fluvoxamine.
Citalopram	CYP2C19	PM	Do not exceed the following daily doses (50% of the standard maximum dose): - Adults up to 65 years: 20 mg as tablets or 16 mg as drops, - Adults 65 years or older: 10 mg as tablets or 8 mg as drops
		IM	Do not exceed the following daily doses: - Adults up to 65 years: 30 mg as tablets or 22 mg as drops, - Adults 65 years or older: 15 mg as tablets or 10 mg as drops
		UM	-
Sertraline	CYP2C19	PM	Do not give doses exceeding 75 mg/day. Guide the dose by response and side effects and/or sertraline plasma concentration.
		IM	-
		UM	-
Paroxetine	CYP2D6	PM	-
		IM	-
		UM	Avoid paroxetine. Antidepressants that are not metabolized by CYP2D6, or to a lesser extent, include for example citalopram or sertraline.
Fluoxetine	CYP2D6	PM	-
		IM	-
		UM	-
Fluvoxamine	CYP2D6	PM	-
		IM	-
		UM	-
Fluvoxamine	CYP2C19	PM	-
		IM	-
		UM	-
Escitalopram/Citalopram	CYP2D6	PM	-
		IM	-
		UM	-
Sertraline	CYP2D6	PM	-
		IM	-
		UM	-

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PM: poor metabolizer, IM: intermediate metabolizer, UM: ultrarapid metabolizer.

^aNo pharmacotherapeutic recommendation: therapy adjustment is not required or beneficial for this phenotype-drug combinations.

The DPWG calculates dose adjustments to optimize treatment based on the difference in exposure with NM. Calculated dose adjustments are subsequently ‘rounded off’ to make application in clinical practice more feasible.

In terms of escitalopram and CYP2C19 UM, the DPWG decided to recommend an alternative antidepressant, because the data to calculate a dose increase were not sufficiently reliable.

For PM, the DPWG recommends a dose reductions to 50% of the normal maximum dose based on the median of the calculated dose adjustment of 54% and the statement in the SmPC of a 50% dose adjustment. For IM, the DPWG recommends a dose reduction to 75% of the normal maximum dose based on a calculated weighted mean of 68%. For prevention of higher plasma concentrations in PM and IM than in NM, only the maximum dose of escitalopram has to be reduced. See Supplementary Table 14 for details.

In terms of citalopram and CYP2C19 PM, the DPWG recommends a dose reduction to 50% of the normal maximum dose based on the 48% calculated from the AUC increase reported by the FDA. The dose reduction based on our own data was considered insufficiently reliable due to the wide variation between the 6 studies (46–108%) and the low number of total PM (n = 32).

For IM, the DPWG recommends a dose reduction to 75% and 65–70% of the normal maximum dose for the tablets and the drops, respectively, based on a calculated weighted mean of 71% of the normal dose. For prevention of higher plasma concentrations in PM and IM than in NM, only the maximum dose of escitalopram has to be reduced. See Supplementary Table 15 for details.

In terms of sertraline and CYP2C19 PM, the DPWG recommends a dose reduction to 37.5% of the normal dose, based on a calculated dose adjustment of 34%. However, as the initial dose for children and certain indications for adults is the lowest commercially available strength of 25 mg, the recommendation for a dose decrease is limited to the maximum dose. See Supplementary Table 16 for details.

In terms of paroxetine and CYP2D6 UM, the DPWG recommends selecting an alternative antidepressant. A dose adjustment could not be calculated because the plasma concentration was below the detection limit in 71% of the UM patients. See Supplementary Table 17 for details.

No therapy adjustments are needed for other gene-drug and phenotype-drug combinations. Supplementary Table 23A through I gives an overview of suggested pop-up texts for electronic prescribing systems for pharmacists and physicians. These can be used to programme alerts into the clinical decision support system.

Implications for clinical practice

Ongoing debate persists whether and which single-drug gene pairs should be implemented into routine care. Points of debate include the amount of evidence that is necessary supporting effectiveness of pre-therapeutic genotyping, cost-effectiveness of PGx testing in the pre-therapeutic setting and its reimbursement [19, 20]. As a consequence drug-gene pairs which are ready for implementation are hampered in the uptake into the clinical practice [1, 21]. In an effort to overcome this inconclusiveness and to direct clinicians on whether or not to order relevant PGx genotyping tests before initiating therapy, the DPWG has developed the clinical implication score. The pre-therapeutic PGx results for a certain drug-gene pair can be scored as: essential, beneficial, or potentially beneficial. The development of these categories and the systematic scoring criteria are discussed elsewhere [22]. In brief, the implications for clinical practice are based on a list of four criteria: the clinical effect associated with the gene-drug interaction, the level of evidence supporting the clinical effect, the effectiveness of the intervention in preventing the clinical effect (i.e., the number needed to genotype) and the PGx information included in the drug-label. The scores provided for each of these criteria by the DPWG can be found in Supplementary Table 24.

As a results, the DPWG concludes pre-therapeutic PGx analysis of CYP2C19 to be potentially beneficial for citalopram, escitalopram, and sertraline. In terms of CYP2D6, pre-therapeutic PGx analysis is considered to be potentially beneficial for paroxetine. This score indicates that genotyping prior to treatment can be considered on an individual patient basis. If, however, the genotype is available, the DPWG recommends adhering to the gene-drug guideline.

Because therapeutic recommendations are lacking for the other gene-drug combinations, pre-therapeutic genotyping provides no benefit for these gene-drug combinations. For this reason, the clinical implication score (with scores ranging from potentially beneficial to essential) is not applicable to these gene-drug combinations.

The DPWG recommendation to consider genotyping on an individual patient basis before initiation of citalopram, escitalopram, sertraline, and paroxetine correlates reasonably well with and can give direction to the recommendation of the Dutch Association for Psychiatry. According to the Dutch Association for Psychiatry, pre-therapeutic genotyping is not recommended, even though it can be considered in patients that already experienced side effects or inefficacy with psychotropic drug use [23].

Differences between available guidelines

To the best of our knowledge, only pharmacogenetics guidelines by the DPWG and the CPIC do concern SSRI. The comparison of the methodologies for grading scientific evidence and strength of the recommendations between the CPIC and DPWG are described elsewhere [24, 25].

For the phenotype-drug combination CYP2C19 UM – citalopram, the CPIC (2015) does recommend to choose an alternative for citalopram, whereas for CYP2C19 UM – sertraline, CYP2D6 PM – paroxetine, and CYP2D6 PM – fluvoxamine, the CPIC (2015) does recommend to optimize the dose or choose an alternative. However, the DPWG states that no action is required for these phenotype-drug combinations. The difference in recommendation for CYP2C19 UM – citalopram can be explained because the DPWG considers the *1/*17 genotype not different enough from the *1/*1 genotype to assign it a separate phenotype, whereas UM + *1/*17 was CPICs definition of UM in 2015. This consideration by the DPWG is based on studies that demonstrated that the effect of *17 is 1) smaller than that of one additional fully functional allele and 2) not correcting the effect of one null allele [26, 27]. Due to the broader definition of UM, the CPIC (2015) recommends an alternative drug for escitalopram in an additional 26–30% of patients in the Netherlands (CYP2C19 *1/*17) (calculation based on the observed allele frequencies in Dutch Whites).

For CYP2C19 IM and PM patients, a reduction to 65–75% and 50% of the normal maximum dose, respectively, is recommended by the DPWG for escitalopram and citalopram. However, the CPIC (2015) solely recommends a 50% reduction of the escitalopram/citalopram starting dose for PM patients.

For CYP2C19 PM patients, the DPWG recommends to not exceed 75 mg/day of sertraline, whereas the CPIC (2015) recommends a consideration of a 50% reduction of the starting dose or an alternative drug. The DPWG does not recommend action in CYP2C19 UM patients, whereas the CPIC (2015) recommends to start with the recommended starting dose, but to consider an alternative drug if the patient does not respond to the recommended maintenance dose.

For CYP2D6 PM patients, the CPIC (2015) recommends to select an alternative drug for paroxetine or, when paroxetine use is warranted, to consider a 50% dose reduction of the starting dose and titrate to response. The DPWG recommends no action. Although the DPWG agreed to the international consensus which allocates gene dose 2.5 to UM [28], at the moment, most Dutch genotyping laboratories cannot distinguish between *1×2/*41 (gene dose 2.5) and *1/*41×2 (gene dose 2), making allocating these genotypes to different predicted phenotypes very impractical.

For CYP2D6 PM patients, the CPIC (2015) recommends a consideration of a 25–50% reduction of the recommended starting dose of fluvoxamine and titration to response. Otherwise, it recommends an alternative drug not metabolized by CYP2D6. The DPWG recommends no action.

Disclaimer

The Pharmacogenetics Working Group of the KNMP (DPWG) formulates the optimal recommendations for each phenotype group based on the available evidence. If this optimal recommendation cannot be followed due to practical restrictions, e.g., therapeutic drug monitoring or a lower dose is not available, then the health care professional should consider the next best option.

Supplementary information

41431_2021_1004_MOESM1_ESM.docx^{(50.3KB, docx)}

Literature review of CYP2C19-escitalopram interactions to support the therapeutic guidelines to choose an alternative or optimize dose.

41431_2021_1004_MOESM2_ESM.docx^{(31.3KB, docx)}

Literature review of CYP2C19-citalopram interactions to support the therapeutic guidelines to optimize dose.

41431_2021_1004_MOESM3_ESM.docx^{(27.8KB, docx)}

Literature review of CYP2C19-sertraline interaction to support the therapeutic guidelines to optimize dose for PM.

41431_2021_1004_MOESM4_ESM.docx^{(33.2KB, docx)}

Literature review of CYP2D6-paroxetine interactions to support the therapeutic guideline to choose an alternative for UM.

41431_2021_1004_MOESM5_ESM.docx^{(23.2KB, docx)}

Literature review of CYP2D6-fluoxetine interactions supporting the absence of a need for therapy adjustment in UM, PM, and IM patients.

41431_2021_1004_MOESM6_ESM.docx^{(30.5KB, docx)}

Literature review of CYP2D6-fluvoxamine interaction supporting the absence of a need for therapy adjustment in UM, PM, and IM patients.

41431_2021_1004_MOESM7_ESM.docx^{(15.4KB, docx)}

Literature review of CYP2C19-fluvoxamine interactions to support the suitability as an alternative in patients with a CYP2C19 gene variant.

41431_2021_1004_MOESM8_ESM.docx^{(35.3KB, docx)}

Literature review of CYP2D6-escitalopram/citalopram interactions to support the suitability as an alternative in patients with a CYP2D6 gene variant.

41431_2021_1004_MOESM9_ESM.docx^{(22.3KB, docx)}

Literature review of CYP2D6-sertraline interactions to support the suitability as an alternative in patients with a CYP2D6 gene variant.

41431_2021_1004_MOESM10_ESM.docx^{(14.9KB, docx)}

The most important CYP2C19 alleles and their predicted enzyme activity.

41431_2021_1004_MOESM11_ESM.docx^{(17.8KB, docx)}

Ethnic variation in prevalence of phenotypes and CYP2C19 allele frequency.

41431_2021_1004_MOESM12_ESM.docx^{(32.3KB, docx)}

CYP2C19 genotype to predicted phenotype translation to be programmed into laboratory information system.

41431_2021_1004_MOESM13_ESM.docx^{(16KB, docx)}

CYP2D6 alleles stratified by gene dose and predicted enzyme activity.

41431_2021_1004_MOESM14_ESM.docx^{(18.1KB, docx)}

Ethnic variation in prevalence of phenotypes and CYP2D6 allele frequency.

41431_2021_1004_MOESM15_ESM.docx^{(45.8KB, docx)}

CYP2D6 genotype to predicted phenotype translation to be programmed into laboratory information system.

41431_2021_1004_MOESM16_ESM.docx^{(25KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2C19 and escitalopram: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM17_ESM.docx^{(19.8KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2C19 and citalopram: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM18_ESM.docx^{(18.5KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2C19 and sertraline: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM19_ESM.docx^{(19.2KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and paroxetine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM20_ESM.docx^{(17.1KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and fluoxetine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM21_ESM.docx^{(17.6KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and fluvoxamine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM22_ESM.docx^{(15.3KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2C19 and fluvoxamine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM23_ESM.docx^{(18.1KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and escitalopram/citalopram: therapeutic recommendation, its rationale, kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM24_ESM.docx^{(15.9KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and sertraline: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM25_ESM.docx^{(54KB, docx)}

Suggested clinical decision support texts for various health care professionals for gene-drug interactions.

41431_2021_1004_MOESM26_ESM.docx^{(16.9KB, docx)}

The clinical implication score of CYP2C19-escitalopram, CYP2C19-citalopram, CYP2C19-sertraline, and CYP2D6-paroxetine is “potentially beneficial”, based on the DPWG criteria and corresponding scores.

41431_2021_1004_MOESM27_ESM.docx^{(28.9KB, docx)}

Detailed description of CYP2C19, CYP2D6, and data and used search-terms for PubMed searches

Acknowledgements

We want to thank Anna de Goede for performing the systematic reviews before April 2007 and Mandy van Rhenen for performing the systematic reviews for CYP2C19/(es)citalopram in 2013 and 2015, CYP2D6/(es)citalopram in 2016, and paroxetine in 2014 and 2016. In addition, we want to thank Leonora Grandia for initiating the pharmacogenetics subject within the Royal Dutch Pharmacists Association and leading this until May 2012. The U-PGx consortium received funding from the European Community’s Horizon 2020 Programme under grant agreement No. 668353 (U-PGx). The DPWG received funding from the Royal Dutch Pharmacists Association.

Author contributions

All authors have contributed to the conception and/or design of the work that led to the submission, the acquisition of data, and/or played an important role in the interpretation of the results. In addition, all authors drafted or revised the manuscript and approved the final version as well as agreed to be accountable for all aspects of the work in ensuring that questions related to the accuracy or integrity of any part of the work are appropiately investigated and resolved.

Data availability

All data and material are either included in the supplementary information or publicly available (i.e., the published articles, PubMed). The guidelines and background information are available on KNMP.nl and will be available on PharmGKB.org.

Competing interests

The authors declare no competing interests.

Ethical approval

This research involves a literature research and no human subjects, human material, or human data. Therefore, no approval by an ethics committee was needed.

Footnotes

Publisher’s note Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Supplementary information

The online version contains supplementary material available at 10.1038/s41431-021-01004-7.

References

1.Swen JJ, Huizinga TW, Gelderblom H, de Vries EG, Assendelft WJ, Kirchheiner J, et al. Translating pharmacogenomics: challenges on the road to the clinic. PLoS Med. 2007;4:1317–24. doi: 10.1371/journal.pmed.0040209. [DOI] [PMC free article] [PubMed] [Google Scholar]
2.Swen JJ, Nijenhuis M, de Boer A, Grandia L, Maitland-van der Zee AH, Mulder H, et al. Pharmacogenetics: from bench to byte-an update of guidelines. Clin Pharm Ther. 2011;89:662–73. doi: 10.1038/clpt.2011.34. [DOI] [PubMed] [Google Scholar]
3.CPIC^® Guideline for Selective Serotonin Reuptake Inhibitors and CYP2D6 and CYP2C19 – CPIC. https://cpicpgx.org/guidelines/guideline-for-selective-serotonin-reuptake-inhibitors-and-cyp2d6-and-cyp2c19/ [Accessed February 2021].
4.van Westrhenen R, van Schaik RHN, van Gelder T, Birkenhager TK, Bakker PR, Houwink EJF, et al. Policy and Practice Review: a First Guideline on the Use of Pharmacogenetics in Clinical Psychiatric Practice. Front Pharmacol. 2021;12:640032. [DOI] [PMC free article] [PubMed]
5.van Westrhenen R, Aitchison KJ, Ingelman-Sundberg M, Jukić MM. Pharmacogenomics of Antidepressant and Antipsychotic Treatment: How Far Have We Got and Where Are We Going? Front Psychiatry. 2020;11:94. [DOI] [PMC free article] [PubMed]
6.CYP2C19 cytochrome P450 family 2 subfamily C member 19 [Homo sapiens (human)] - Gene - NCBI. https://www.ncbi.nlm.nih.gov/gene/1557.
7.Wedlund PJ. The CYP2C19 enzyme polymorphism. Pharmacology. 2000;61:174–83. doi: 10.1159/000028398. [DOI] [PubMed] [Google Scholar]
8.Sim SC, Risinger C, Dahl ML, Aklillu E, Christensen M, Bertilsson L, et al. A common novel CYP2C19 gene variant causes ultrarapid drug metabolism relevant for the drug response to proton pump inhibitors and antidepressants. Clin Pharm Ther. 2006;79:103–13. doi: 10.1016/j.clpt.2005.10.002. [DOI] [PubMed] [Google Scholar]
9.Pharmacogene Variation Consortium: CYP2C19. https://www.pharmvar.org/gene/CYP2C19. [Accessed June 2019].
10.Scott SA, Sangkuhl K, Stein CM, Hulot JS, Mega JL, Roden DM, et al. Clinical Pharmacogenetics Implementation Consortium guidelines for CYP2C19 genotype and clopidogrel therapy: 2013 update. Clin Pharm Ther. 2013;94:317–23. doi: 10.1038/clpt.2013.105. [DOI] [PMC free article] [PubMed] [Google Scholar]
11.Kurzawski M, Gawrońska-Szklarz B, Wrześniewska J, Siuda A, Starzyńska T, Droździk M. Effect of CYP2C19*17 gene variant on Helicobacter pylori eradication in peptic ulcer patients. Eur J Clin Pharm. 2006;62:877–80. doi: 10.1007/s00228-006-0183-2. [DOI] [PubMed] [Google Scholar]
12.Sugimoto K, Uno T, Yamazaki H, Tateishi T. Limited frequency of the CYP2C19*17 allele and its minor role in a Japanese population. Br J Clin Pharm. 2008;65:437–9. doi: 10.1111/j.1365-2125.2007.03057.x. [DOI] [PMC free article] [PubMed] [Google Scholar]
13.Matic M, Nijenhuis M, Soree B, de Boer-Veger NJ, Buunk AM, Houwink EJF, et al. Dutch Pharmacogenetics Working Group (DPWG) guideline for the gene-drug interaction between CYP2D6 and opioids (codeine, tramadol and oxycodone). Eur J Hum Genet. 2021. Online ahead of print. [DOI] [PMC free article] [PubMed]
14.Hiemke C, Bergemann N, Clement HW, Conca A, Deckert J, Domschke K, et al. Consensus Guidelines for Therapeutic Drug Monitoring in Neuropsychopharmacology: Update 2017. Pharmacopsychiatry. 2018;51:9–62. doi: 10.1055/s-0043-116492. [DOI] [PubMed] [Google Scholar]
15.Meyer JH, Wilson AA, Sagrati S, Hussey D, Carella A, Potter WZ, et al. Serotonin transporter occupancy of five selective serotonin reuptake inhibitors at different doses: an [11C]DASB positron emission tomography study. Am J Psychiatry. 2004;161:826–35. doi: 10.1176/appi.ajp.161.5.826. [DOI] [PubMed] [Google Scholar]
16.Alfaro CL, Lam YW, Simpson J, Ereshefsky L. CYP2D6 inhibition by fluoxetine, paroxetine, sertraline, and venlafaxine in a crossover study: intraindividual variability and plasma concentration correlations. J Clin Pharm. 2000;40:58–66. doi: 10.1177/009127000004000108. [DOI] [PubMed] [Google Scholar]
17.Alfaro CL, Lam YW, Simpson J, Ereshefsky L. CYP2D6 status of extensive metabolizers after multiple-dose fluoxetine, fluvoxamine, paroxetine, or sertraline. J Clin Psychopharmacol. 1999;19:155–63. doi: 10.1097/00004714-199904000-00011. [DOI] [PubMed] [Google Scholar]
18.Swen JJ, Wilting I, Goede AL De, Grandia L, Mulder H, Touw DJ, et al. Pharmacogenetics: From bench to byte. Vol. 83, Clinical Pharmacology and Therapeutics. Nature Publishing Group; 2008;83:781–7. [DOI] [PubMed]
19.Karamperis K, Koromina M, Papantoniou P, Skokou M, Kanellakis F, Mitropoulos K, et al. Economic evaluation in psychiatric pharmacogenomics: a systematic review. Pharmacogenomics J. 2021;21:533–41. doi: 10.1038/s41397-021-00249-1. [DOI] [PubMed] [Google Scholar]
20.Simeonidis S, Koutsilieri S, Vozikis A, Cooper DN, Mitropoulou C, Patrinos GP. Application of Economic Evaluation to Assess Feasibility for Reimbursement of Genomic Testing as Part of Personalized Medicine Interventions. Front Pharmacol. 2019;10:830. [DOI] [PMC free article] [PubMed]
21.Lunenburg CATC, Henricks LM, Guchelaar HJ, Swen JJ, Deenen MJ, Schellens JHM, et al. Prospective DPYD genotyping to reduce the risk of fluoropyrimidine-induced severe toxicity: ready for prime time. Eur J Cancer. 2016;54:40–8. doi: 10.1016/j.ejca.2015.11.008. [DOI] [PubMed] [Google Scholar]
22.Swen JJ, Nijenhuis M, van Rhenen M, de Boer-Veger NJ, Buunk AM, Houwink EJF, et al. Pharmacogenetic Information in Clinical Guidelines: The European Perspective. Clin Pharm Ther. 2018;103:795–801. doi: 10.1002/cpt.1049. [DOI] [PubMed] [Google Scholar]
23.Leidraad farmacogenetica voor de dagelijkse psychiatrische praktijk. https://www.nvvp.net/website/nieuws/2020/leidraad-farmacogenetica-voor-de-dagelijkse-psychiatrische-praktijk.
24.Bank PCD, Caudle KE, Swen JJ, Gammal RS, Whirl-Carrillo M, Klein TE, et al. Comparison of the Guidelines of the Clinical Pharmacogenetics Implementation Consortium and the Dutch Pharmacogenetics Working Group. Clin Pharmacol Ther Nat Publ Group. 2018;103:599–618. doi: 10.1002/cpt.762. [DOI] [PMC free article] [PubMed] [Google Scholar]
25.Abdullah-Koolmees H, van Keulen AM, Nijenhuis M, Deneer VHM. Pharmacogenetics Guidelines: Overview and Comparison of the DPWG, CPIC, CPNDS, and RNPGx Guidelines. Front Pharmacol. 2021;11:595219. [DOI] [PMC free article] [PubMed]
26.Rudberg I, Hermann M, Refsum H, Molden E. Serum concentrations of sertraline and N-desmethyl sertraline in relation to CYP2C19 genotype in psychiatric patients. Eur J Clin Pharm. 2008;64:1181–8. doi: 10.1007/s00228-008-0533-3. [DOI] [PubMed] [Google Scholar]
27.Rudberg I, Mohebi B, Hermann M, Refsum H, Molden E. Impact of the ultrarapid CYP2C19*17 allele on serum concentration of escitalopram in psychiatric patients. Clin Pharm Ther. 2008;83:322–7. doi: 10.1038/sj.clpt.6100291. [DOI] [PubMed] [Google Scholar]
28.Caudle KE, Sangkuhl K, Whirl-Carrillo M, Swen JJ, Haidar CE, Klein TE, et al. Standardizing CYP2D6 Genotype to Phenotype Translation: Consensus Recommendations from the Clinical Pharmacogenetics Implementation Consortium and Dutch Pharmacogenetics Working Group. Clin Transl Sci. 2020;13:116–24. doi: 10.1111/cts.12692. [DOI] [PMC free article] [PubMed] [Google Scholar]

Associated Data

This section collects any data citations, data availability statements, or supplementary materials included in this article.

Supplementary Materials

41431_2021_1004_MOESM1_ESM.docx^{(50.3KB, docx)}

Literature review of CYP2C19-escitalopram interactions to support the therapeutic guidelines to choose an alternative or optimize dose.

41431_2021_1004_MOESM2_ESM.docx^{(31.3KB, docx)}

Literature review of CYP2C19-citalopram interactions to support the therapeutic guidelines to optimize dose.

41431_2021_1004_MOESM3_ESM.docx^{(27.8KB, docx)}

Literature review of CYP2C19-sertraline interaction to support the therapeutic guidelines to optimize dose for PM.

41431_2021_1004_MOESM4_ESM.docx^{(33.2KB, docx)}

Literature review of CYP2D6-paroxetine interactions to support the therapeutic guideline to choose an alternative for UM.

41431_2021_1004_MOESM5_ESM.docx^{(23.2KB, docx)}

Literature review of CYP2D6-fluoxetine interactions supporting the absence of a need for therapy adjustment in UM, PM, and IM patients.

41431_2021_1004_MOESM6_ESM.docx^{(30.5KB, docx)}

Literature review of CYP2D6-fluvoxamine interaction supporting the absence of a need for therapy adjustment in UM, PM, and IM patients.

41431_2021_1004_MOESM7_ESM.docx^{(15.4KB, docx)}

Literature review of CYP2C19-fluvoxamine interactions to support the suitability as an alternative in patients with a CYP2C19 gene variant.

41431_2021_1004_MOESM8_ESM.docx^{(35.3KB, docx)}

Literature review of CYP2D6-escitalopram/citalopram interactions to support the suitability as an alternative in patients with a CYP2D6 gene variant.

41431_2021_1004_MOESM9_ESM.docx^{(22.3KB, docx)}

Literature review of CYP2D6-sertraline interactions to support the suitability as an alternative in patients with a CYP2D6 gene variant.

41431_2021_1004_MOESM10_ESM.docx^{(14.9KB, docx)}

The most important CYP2C19 alleles and their predicted enzyme activity.

41431_2021_1004_MOESM11_ESM.docx^{(17.8KB, docx)}

Ethnic variation in prevalence of phenotypes and CYP2C19 allele frequency.

41431_2021_1004_MOESM12_ESM.docx^{(32.3KB, docx)}

CYP2C19 genotype to predicted phenotype translation to be programmed into laboratory information system.

41431_2021_1004_MOESM13_ESM.docx^{(16KB, docx)}

CYP2D6 alleles stratified by gene dose and predicted enzyme activity.

41431_2021_1004_MOESM14_ESM.docx^{(18.1KB, docx)}

Ethnic variation in prevalence of phenotypes and CYP2D6 allele frequency.

41431_2021_1004_MOESM15_ESM.docx^{(45.8KB, docx)}

CYP2D6 genotype to predicted phenotype translation to be programmed into laboratory information system.

41431_2021_1004_MOESM16_ESM.docx^{(25KB, docx)}

41431_2021_1004_MOESM17_ESM.docx^{(19.8KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2C19 and citalopram: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM18_ESM.docx^{(18.5KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2C19 and sertraline: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM19_ESM.docx^{(19.2KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and paroxetine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM20_ESM.docx^{(17.1KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and fluoxetine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM21_ESM.docx^{(17.6KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and fluvoxamine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM22_ESM.docx^{(15.3KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2C19 and fluvoxamine: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM23_ESM.docx^{(18.1KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and escitalopram/citalopram: therapeutic recommendation, its rationale, kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM24_ESM.docx^{(15.9KB, docx)}

Dutch Pharmacogenetics Working Group (DPWG) Guideline for CYP2D6 and sertraline: therapeutic recommendation and its rationale, and the kinetic and clinical consequences for each predicted phenotype

41431_2021_1004_MOESM25_ESM.docx^{(54KB, docx)}

Suggested clinical decision support texts for various health care professionals for gene-drug interactions.

41431_2021_1004_MOESM26_ESM.docx^{(16.9KB, docx)}

41431_2021_1004_MOESM27_ESM.docx^{(28.9KB, docx)}

Detailed description of CYP2C19, CYP2D6, and data and used search-terms for PubMed searches

Data Availability Statement

[CR1] 1.Swen JJ, Huizinga TW, Gelderblom H, de Vries EG, Assendelft WJ, Kirchheiner J, et al. Translating pharmacogenomics: challenges on the road to the clinic. PLoS Med. 2007;4:1317–24. doi: 10.1371/journal.pmed.0040209. [DOI] [PMC free article] [PubMed] [Google Scholar]

[CR2] 2.Swen JJ, Nijenhuis M, de Boer A, Grandia L, Maitland-van der Zee AH, Mulder H, et al. Pharmacogenetics: from bench to byte-an update of guidelines. Clin Pharm Ther. 2011;89:662–73. doi: 10.1038/clpt.2011.34. [DOI] [PubMed] [Google Scholar]

[CR3] 3.CPIC^® Guideline for Selective Serotonin Reuptake Inhibitors and CYP2D6 and CYP2C19 – CPIC. https://cpicpgx.org/guidelines/guideline-for-selective-serotonin-reuptake-inhibitors-and-cyp2d6-and-cyp2c19/ [Accessed February 2021].

[CR4] 4.van Westrhenen R, van Schaik RHN, van Gelder T, Birkenhager TK, Bakker PR, Houwink EJF, et al. Policy and Practice Review: a First Guideline on the Use of Pharmacogenetics in Clinical Psychiatric Practice. Front Pharmacol. 2021;12:640032. [DOI] [PMC free article] [PubMed]

[CR5] 5.van Westrhenen R, Aitchison KJ, Ingelman-Sundberg M, Jukić MM. Pharmacogenomics of Antidepressant and Antipsychotic Treatment: How Far Have We Got and Where Are We Going? Front Psychiatry. 2020;11:94. [DOI] [PMC free article] [PubMed]

[CR6] 6.CYP2C19 cytochrome P450 family 2 subfamily C member 19 [Homo sapiens (human)] - Gene - NCBI. https://www.ncbi.nlm.nih.gov/gene/1557.

[CR7] 7.Wedlund PJ. The CYP2C19 enzyme polymorphism. Pharmacology. 2000;61:174–83. doi: 10.1159/000028398. [DOI] [PubMed] [Google Scholar]

[CR8] 8.Sim SC, Risinger C, Dahl ML, Aklillu E, Christensen M, Bertilsson L, et al. A common novel CYP2C19 gene variant causes ultrarapid drug metabolism relevant for the drug response to proton pump inhibitors and antidepressants. Clin Pharm Ther. 2006;79:103–13. doi: 10.1016/j.clpt.2005.10.002. [DOI] [PubMed] [Google Scholar]

[CR9] 9.Pharmacogene Variation Consortium: CYP2C19. https://www.pharmvar.org/gene/CYP2C19. [Accessed June 2019].

[CR10] 10.Scott SA, Sangkuhl K, Stein CM, Hulot JS, Mega JL, Roden DM, et al. Clinical Pharmacogenetics Implementation Consortium guidelines for CYP2C19 genotype and clopidogrel therapy: 2013 update. Clin Pharm Ther. 2013;94:317–23. doi: 10.1038/clpt.2013.105. [DOI] [PMC free article] [PubMed] [Google Scholar]

[CR11] 11.Kurzawski M, Gawrońska-Szklarz B, Wrześniewska J, Siuda A, Starzyńska T, Droździk M. Effect of CYP2C19*17 gene variant on Helicobacter pylori eradication in peptic ulcer patients. Eur J Clin Pharm. 2006;62:877–80. doi: 10.1007/s00228-006-0183-2. [DOI] [PubMed] [Google Scholar]

[CR12] 12.Sugimoto K, Uno T, Yamazaki H, Tateishi T. Limited frequency of the CYP2C19*17 allele and its minor role in a Japanese population. Br J Clin Pharm. 2008;65:437–9. doi: 10.1111/j.1365-2125.2007.03057.x. [DOI] [PMC free article] [PubMed] [Google Scholar]

[CR13] 13.Matic M, Nijenhuis M, Soree B, de Boer-Veger NJ, Buunk AM, Houwink EJF, et al. Dutch Pharmacogenetics Working Group (DPWG) guideline for the gene-drug interaction between CYP2D6 and opioids (codeine, tramadol and oxycodone). Eur J Hum Genet. 2021. Online ahead of print. [DOI] [PMC free article] [PubMed]

[CR14] 14.Hiemke C, Bergemann N, Clement HW, Conca A, Deckert J, Domschke K, et al. Consensus Guidelines for Therapeutic Drug Monitoring in Neuropsychopharmacology: Update 2017. Pharmacopsychiatry. 2018;51:9–62. doi: 10.1055/s-0043-116492. [DOI] [PubMed] [Google Scholar]

[CR15] 15.Meyer JH, Wilson AA, Sagrati S, Hussey D, Carella A, Potter WZ, et al. Serotonin transporter occupancy of five selective serotonin reuptake inhibitors at different doses: an [11C]DASB positron emission tomography study. Am J Psychiatry. 2004;161:826–35. doi: 10.1176/appi.ajp.161.5.826. [DOI] [PubMed] [Google Scholar]

[CR16] 16.Alfaro CL, Lam YW, Simpson J, Ereshefsky L. CYP2D6 inhibition by fluoxetine, paroxetine, sertraline, and venlafaxine in a crossover study: intraindividual variability and plasma concentration correlations. J Clin Pharm. 2000;40:58–66. doi: 10.1177/009127000004000108. [DOI] [PubMed] [Google Scholar]

[CR17] 17.Alfaro CL, Lam YW, Simpson J, Ereshefsky L. CYP2D6 status of extensive metabolizers after multiple-dose fluoxetine, fluvoxamine, paroxetine, or sertraline. J Clin Psychopharmacol. 1999;19:155–63. doi: 10.1097/00004714-199904000-00011. [DOI] [PubMed] [Google Scholar]

[CR18] 18.Swen JJ, Wilting I, Goede AL De, Grandia L, Mulder H, Touw DJ, et al. Pharmacogenetics: From bench to byte. Vol. 83, Clinical Pharmacology and Therapeutics. Nature Publishing Group; 2008;83:781–7. [DOI] [PubMed]

[CR19] 19.Karamperis K, Koromina M, Papantoniou P, Skokou M, Kanellakis F, Mitropoulos K, et al. Economic evaluation in psychiatric pharmacogenomics: a systematic review. Pharmacogenomics J. 2021;21:533–41. doi: 10.1038/s41397-021-00249-1. [DOI] [PubMed] [Google Scholar]

[CR20] 20.Simeonidis S, Koutsilieri S, Vozikis A, Cooper DN, Mitropoulou C, Patrinos GP. Application of Economic Evaluation to Assess Feasibility for Reimbursement of Genomic Testing as Part of Personalized Medicine Interventions. Front Pharmacol. 2019;10:830. [DOI] [PMC free article] [PubMed]

[CR21] 21.Lunenburg CATC, Henricks LM, Guchelaar HJ, Swen JJ, Deenen MJ, Schellens JHM, et al. Prospective DPYD genotyping to reduce the risk of fluoropyrimidine-induced severe toxicity: ready for prime time. Eur J Cancer. 2016;54:40–8. doi: 10.1016/j.ejca.2015.11.008. [DOI] [PubMed] [Google Scholar]

[CR22] 22.Swen JJ, Nijenhuis M, van Rhenen M, de Boer-Veger NJ, Buunk AM, Houwink EJF, et al. Pharmacogenetic Information in Clinical Guidelines: The European Perspective. Clin Pharm Ther. 2018;103:795–801. doi: 10.1002/cpt.1049. [DOI] [PubMed] [Google Scholar]

[CR23] 23.Leidraad farmacogenetica voor de dagelijkse psychiatrische praktijk. https://www.nvvp.net/website/nieuws/2020/leidraad-farmacogenetica-voor-de-dagelijkse-psychiatrische-praktijk.

[CR24] 24.Bank PCD, Caudle KE, Swen JJ, Gammal RS, Whirl-Carrillo M, Klein TE, et al. Comparison of the Guidelines of the Clinical Pharmacogenetics Implementation Consortium and the Dutch Pharmacogenetics Working Group. Clin Pharmacol Ther Nat Publ Group. 2018;103:599–618. doi: 10.1002/cpt.762. [DOI] [PMC free article] [PubMed] [Google Scholar]

[CR25] 25.Abdullah-Koolmees H, van Keulen AM, Nijenhuis M, Deneer VHM. Pharmacogenetics Guidelines: Overview and Comparison of the DPWG, CPIC, CPNDS, and RNPGx Guidelines. Front Pharmacol. 2021;11:595219. [DOI] [PMC free article] [PubMed]

[CR26] 26.Rudberg I, Hermann M, Refsum H, Molden E. Serum concentrations of sertraline and N-desmethyl sertraline in relation to CYP2C19 genotype in psychiatric patients. Eur J Clin Pharm. 2008;64:1181–8. doi: 10.1007/s00228-008-0533-3. [DOI] [PubMed] [Google Scholar]

[CR27] 27.Rudberg I, Mohebi B, Hermann M, Refsum H, Molden E. Impact of the ultrarapid CYP2C19*17 allele on serum concentration of escitalopram in psychiatric patients. Clin Pharm Ther. 2008;83:322–7. doi: 10.1038/sj.clpt.6100291. [DOI] [PubMed] [Google Scholar]

[CR28] 28.Caudle KE, Sangkuhl K, Whirl-Carrillo M, Swen JJ, Haidar CE, Klein TE, et al. Standardizing CYP2D6 Genotype to Phenotype Translation: Consensus Recommendations from the Clinical Pharmacogenetics Implementation Consortium and Dutch Pharmacogenetics Working Group. Clin Transl Sci. 2020;13:116–24. doi: 10.1111/cts.12692. [DOI] [PMC free article] [PubMed] [Google Scholar]

PERMALINK

Dutch Pharmacogenetics Working Group (DPWG) guideline for the gene-drug interaction between CYP2C19 and CYP2D6 and SSRIs

Jurriaan M J L Brouwer

Marga Nijenhuis

Bianca Soree

Henk-Jan Guchelaar

Jesse J Swen

Ron H N van Schaik

Jan van der Weide

Gerard A P J M Rongen

Anne-Marie Buunk

Nienke J de Boer-Veger

Elisa J F Houwink

Roos van Westrhenen

Bob Wilffert

Vera H M Deneer

Hans Mulder

Abstract

Introduction

Drugs: selective serotonin reuptake inhibitors

Gene: CYP2C19 (Cytochrome P450 family 2 subfamily C member 19)

Translation of genotype to predicted phenotype

Table 1.

Gene: CYP2D6 (Cytochrome P450 family 2 subfamily D member 6)

Gene-drug interaction

Pharmacological mechanism

Supporting body of evidence

General conclusions of evidence

CYP2C19 – Escitalopram

CYP2C19 – Citalopram

CYP2C19 – Sertraline

CYP2D6 – Paroxetine

CYP2D6 – Fluoxetine

CYP2D6 – Fluvoxamine

CYP2C19 – Fluvoxamine, CYP2D6 – Escitalopram/citalopram, and CYP2D6 – Sertraline

Pharmacotherapeutic recommendations

Table 2.

Implications for clinical practice

Differences between available guidelines

Disclaimer

Supplementary information

Acknowledgements

Author contributions

Data availability

Competing interests

Ethical approval

Footnotes

Supplementary information

References

Associated Data

Supplementary Materials

Data Availability Statement

ACTIONS

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RESOURCES

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