Clinical Pharmacogenetics Implementation Consortium (CPIC) Guideline for CYP2C9 and Nonsteroidal Anti-inflammatory Drugs

Katherine N Theken; Craig R Lee; Li Gong; Kelly E Caudle; Christine M Formea; Andrea Gaedigk; Teri E Klein; José A G Agúndez; Tilo Grosser

doi:10.1002/cpt.1830

. Author manuscript; available in PMC: 2021 Aug 1.

Published in final edited form as: Clin Pharmacol Ther. 2020 Apr 28;108(2):191–200. doi: 10.1002/cpt.1830

Clinical Pharmacogenetics Implementation Consortium (CPIC) Guideline for CYP2C9 and Nonsteroidal Anti-inflammatory Drugs

Katherine N Theken ¹, Craig R Lee ², Li Gong ³, Kelly E Caudle ⁴, Christine M Formea ^5,⁶, Andrea Gaedigk ^7,⁸, Teri E Klein ³, José A G Agúndez ⁹, Tilo Grosser ¹

PMCID: PMC8080882 NIHMSID: NIHMS1687646 PMID: 32189324

Abstract

Nonsteroidal anti-inflammatory drugs (NSAIDs) are among the most commonly used analgesics due to their lack of addictive potential. However, NSAIDs have the potential to cause serious gastrointestinal, renal, and cardiovascular adverse events. CYP2C9 polymorphisms influence metabolism and clearance of several drugs in this class, thereby affecting drug exposure and potentially safety. We summarize evidence from the published literature supporting these associations and provide therapeutic recommendations for NSAIDs based on CYP2C9 genotype (updates at www.cpicpgx.org).

Keywords: CPIC, pharmacogenetics, pharmacogenomics, NSAID, CYP2C9, celecoxib, diclofenac, flurbiprofen, ibuprofen, meloxicam, naproxen, piroxicam, tenoxicam, sulindac, nabumetone, indomethacin

INTRODUCTION

The purpose of this guideline is to provide information for the interpretation of CYP2C9 genotype tests so that the results can guide dosing and/or use of nonsteroidal anti-inflammatory drugs (NSAIDs). Detailed guidelines for use of NSAIDs as well as cost effectiveness of CYP2C9 genotyping are beyond the scope of this document. Clinical Pharmacogenetics Implementation Consortium (CPIC) guidelines are periodically updated at www.cpicpgx.org/guidelines/.

FOCUSED LITERATURE REVIEW

A systematic literature review focused on CYP2C9 genotype and NSAID (celecoxib, diclofenac, flurbiprofen, ibuprofen, indomethacin, lornoxicam, meloxicam, nabumetone, naproxen, piroxicam, tenoxicam, and sulindac) use and CYP2C8 genotype and ibuprofen, piroxicam and diclofenac use was conducted (details in Supplemental Material). Evidence summarized in Tables S1 to S10.

GENE: CYP2C9

Hepatic CYP2C9 enzyme contributes to the metabolism of many drugs, including several NSAIDs (celecoxib, diclofenac, flurbiprofen, indomethacin, ibuprofen, lornoxicam, meloxicam, nabumetone, naproxen, piroxicam, and tenoxicam). The CYP2C9 gene is highly polymorphic, with at least 61 variant alleles and multiple sub-alleles (see CYP2C9 Allele Definition Table in references (1, 2)). Differences in allele frequencies have been observed across multiple geographically, racially and ethnically diverse groups (see CYP2C9 Allele Frequency Table in references (1, 2)). The most commonly reported alleles are categorized into functional groups as follows: normal function (e.g., CYP2C9*1), decreased function (e.g., CYP2C9*2, *5, *8, *11), and no function (e.g., CYP2C9*3, *6, *13). Allele function assignments, have been made based on available in vitro and in vivo data, with consideration for their clinical actionability (1, 2). The two most extensively studied variants are CYP2C9*2 (p.R144C; rs1799853) and CYP2C9*3 (p.I359L; rs1057910) (3). In vitro and clinical studies suggest that the catalytic activity of CYP2C9 decreased function and no function alleles is substrate-dependent. Therefore, assigning function to CYP2C9 alleles requires careful evaluation of individual drugs.

Genetic Test Interpretation

Most clinical laboratories reporting CYP2C9 genotype use the star (*) allele nomenclature, in which each allele is defined by a genotype at one or more specific single-nucleotide polymorphisms (SNPs) with variable enzyme activity. The star (*)-allele nomenclature for CYP2C9 is found at the Pharmacogene Variation (PharmVar) Consortium website (https://www.pharmvar.org/gene/CYP2C9). The combination of alleles is used to determine a patient’s diplotype (often also referred to as genotype), which can then be used to infer an individual’s predicted metabolizer phenotype (Table 1; CYP2C9 diplotype to phenotype table (1, 2)). Each allele functional status is assigned an activity value ranging from 0 to 1 (e.g., 0 for no function, 0.5 for decreased, and 1.0 for normal function), which are summed to calculate the activity score (AS) for each diplotype (1, 2). The CYP2C9 AS has been translated into the phenotype classification system as follows: individuals with an AS of 0 or 0.5 are poor metabolizers (PMs), those with a score of 1 or 1.5 are intermediate metabolizers (IMs), and those with a score of 2 are normal metabolizers (NMs) (Table 1; CYP2C9 diplotype to phenotype table (1, 2)). Because reference laboratories providing clinical CYP2C9 genotyping may use varying methods to assign phenotypes, it is advisable to note a patient’s CYP2C9 diplotype and to refer to the CYP2C9 Diplotype to Phenotype Table (1, 2) online for a complete list of possible diplotypes and phenotype assignments before making therapeutic decisions about NSAID therapy.

TABLE 1.

ASSIGNMENT OF LIKELY CYP2C9 PHENOTYPES BASED ON GENOTYPES

Likely Phenotype^a,b	Activity Score	Genotypes	Examples of diplotypes
Normal Metabolizer	2	An individual carrying two normal function alleles	1/1
Intermediate Metabolizer	1.5 1	An individual carrying one normal function allele plus one decreased function allele; OR one normal function allele plus one no function allele OR two decreased function alleles	1/2 1/3, 2/2
Poor Metabolizer	0.5 0	An individual carrying one no function allele plus one decreased function allele; OR two no function alleles	2/3 3/3
Indeterminate	n/a	An individual carrying allele combinations with uncertain and/or unknown function alleles	1/7, 1/10, 7/10, 1/57

Open in a new tab

Assignment of allele function and associated citations can be found at https://www.pharmgkb.org/page/cyp2c9RefMaterials (see CYP2C9 Allele Definition Table and CYP2C9 Allele Functionality Table in references (1, 2)). For a complete list of CYP2C9 diplotypes and resulting phenotypes, see the CYP2C9 Genotype to Phenotype Table in references (1, 2).

See the CYP2C9 Frequency Table in references (1, 2) for population-specific allele and phenotype frequencies.

Of note, Table 1 denotes a change to the prior genotype to phenotype translation tables (4) for diplotypes containing CYP2C9*2 and other decreased function alleles. The phenotype group for CYP2C9*2/*2 (AS=1) is now translated into the IM phenotype group (originally translated to PM). This change is based on data from multiple substrates (flurbiprofen, celecoxib, phenytoin, and warfarin) showing a similar effect of CYP2C9*1/*3 (AS=1) and CYP2C9*2/*2 on metabolic ratio and dose requirements (warfarin) (5–7). Furthermore, CYP2C9*3 and alleles with similar clinical effect and function were assigned a clinical function as ‘no function’ with an activity value of 0 (previously decreased function). This is based on CYP2C9*3/*3 which is the diplotype with the lowest clinically actionable activity; thus, the CYP2C9*3 allele receives a ‘no function’ assignment. Other alleles with similarly low function will also be classified as ‘no function’.

Currently, clinical laboratories rarely sequence the entire CYP2C9 gene or interrogate every known variant position. Instead, they typically test for variants that are used to determine common haplotypes (also referred to as alleles) using the star-allele (*) nomenclature system. Tables on the CPIC and PharmGKB websites contain a list of CYP2C9 alleles, the specific combination of variants that can be used to determine each allele, allele functional status, and frequency across major ethnic populations as reported in the literature (1, 2).

Available Genetic Test Options

See the Genetic Testing Registry (www.ncbi.nlm.nih.gov/gtr/) for more information on commercially available clinical testing options.

Incidental Findings

No diseases or conditions have been consistently or strongly linked to variation in CYP2C9 independent of drug metabolism and response. CYP2C9 IMs and PMs may be predisposed to serious bleeding during warfarin therapy and increased risk of phenytoin-related toxicities (4, 8).

Other Considerations

CYP2C9 is located within a cluster of CYP2C genes (CYP2C18, CYP2C19, CYP2C9, and CYP2C8) on chromosome 10 (Figure S1), which evolved from a common ancestral CYP gene through duplication events (9). Importantly, the CYP2C9*2 allele is in strong linkage disequilibrium with the CYP2C8*3 allele (Table S11), such that more than 80% of individuals who carry the CYP2C9*2 allele also carry the CYP2C8*3 allele in many populations (10). This may be of clinical relevance for drugs that are substrates for both CYP2C8 and CYP2C9 such as diclofenac and ibuprofen.

DRUG: NSAIDs

Background

NSAIDs are among the most commonly used analgesics due to their lack of addictive potential (11). They are also one of the most diverse classes of clinically available drugs, with more than 40 chemically distinct compounds marketed world-wide. The principal therapeutic effect of NSAIDs occurs via inhibition of prostaglandin biosynthesis from arachidonic acid by the prostaglandin G/H synthases 1 and 2, also known as cyclooxygenases (COX) (12). Most NSAIDs are reversible inhibitors of both the COX-1 and COX-2 isoforms. Celecoxib, meloxicam, and diclofenac are selective COX-2 inhibitors.

Millions of older adults consume NSAIDs regularly for chronic pain (13), while short term use is prevalent in those experiencing acute pain and musculoskeletal injuries (14, 15). NSAIDs are commonly used in pediatric patients to reduce fever and ameliorate pain and in preterm infants or neonates with patent ductus arteriosus as an attempt to induce closure of the ductus.

Hepatic biotransformation, often via cytochrome P450 isoforms CYP2C9, 1A2, and 3A4 (Table S12), and renal excretion are the principal routes of clearance of the majority of NSAIDs. The activity of CYP enzymes is influenced by genetic variation, age, gender, circadian variation, disease, and interacting drugs that are CYP substrates, inhibitors or inducers (16). Thus, variability in the metabolism of NSAIDs can have a considerable impact on drug exposure. Several NSAIDs undergo enterohepatic recycling, thus amplifying interindividual variability in drug exposure.

While several NSAIDs are considered safe for over-the-counter use, they have the potential to cause serious complications, including gastrointestinal (GI) bleeding (1–2% per year of regular users), hypertension (up to 5% per year of regular users), myocardial infarction (up to 1% per year), heart failure (up to 1% per year) and renal damage; arrhythmias and sudden cardiac death have also been observed in rare cases (11). With the large population exposure to NSAIDs, these adverse events may have considerable public health and economic impacts, although this is difficult to quantify particularly for cardiovascular adverse effects, given the background prevalence of cardiovascular disease in the general population (17).

Individual risk factors, such as older age, concomitant drug use, or preexisting disease, have been associated with the occurrence of adverse events; however, our understanding of the molecular mechanisms - including genetic predisposition - that result in complications in some patients, but not others, is limited. Importantly, NSAID adverse events are largely on-target adverse events caused by the inhibition of COX-1 or COX-2 in tissues in which they fulfill physiological functions such as the GI tract, kidney and cardiovascular system (18), resulting in an increased risk of complications with increased drug doses or exposure (12). This has been borne out in a meta-analysis that demonstrated the dose-dependency of cardiovascular complications related to celecoxib (19).

Linking Genetic Variability to Variability in Drug-related Phenotypes

Substantial evidence links CYP2C9 genotypes with phenotypic variability in CYP2C9 metabolism and plasma NSAID concentrations, with the majority of studies conducted in healthy volunteers (Tables S1 to S9). Application of a grading system to evidence linking genotypic with pharmacokinetic variability indicates a moderate to high quality of evidence for most NSAIDs. The quality of evidence linking genotype to NSAID therapeutic response and adverse events was graded as weak in most cases (Tables S1 to S9). See the Supplemental Material for additional summaries for each drug covered in this guideline. Although clinical evidence linking genetic variation in CYP2C9 to an increased rate of adverse events with NSAIDs use is scarce, several studies have established an association between CYP2C9 decreased function and no function alleles and elevated NSAID exposure (Figure 1 and Figure S2). Because most NSAID adverse events are dose-dependent, on-target adverse events involving COX inhibition (19–23) it is reasonable to assume that elevated exposure increases the risk of adverse events.

Figure 1. — Sample sizes and reported area under the curve (AUC) data were extracted from clinical pharmacokinetic studies reviewed for this guideline. Results are expressed as the ratio of mean AUC for variant allele carriers to *CYP2C9*1/*1* controls. Overall effects of individual drugs were only estimated using a random effects model when three or more studies were available for analysis. References shown in parenthesis and methodological details are provided in the Supplemental Material.

Therapeutic Recommendations

NSAIDs may be used on a chronic, short-term, or as needed (PRN) basis. While data on risks associated with short-term or PRN NSAID consumption versus chronic use are limited, the risks of upper gastrointestinal bleeding and myocardial infarction are thought to be similar among new and chronic NSAID users (24, 25). Thus, these recommendations can be considered and appliedregardless of treatment duration. Also of note, as some short-acting NSAIDs (e.g., low dose ibuprofen) can be purchased over-the-counter in some countries, clinicians need to be aware that these recommendations also apply to these drugs.

CYP2C9 IM and PM phenotypes affect systemic plasma concentrations of NSAIDs by decreasing metabolic clearance and consequently prolonging plasma elimination half-life. Therefore, therapeutic recommendations are broadly organized according to the NSAID plasma elimination half-life in NMs. Where more than two studies reported plasma concentration area-under-the-curve (AUC), a meta-analysis was conducted to estimate the average impact of CYP2C9 genotype on drug exposure (Figure 1 and Figures S2 to S4).

Celecoxib, flurbiprofen, ibuprofen, lornoxicam.

Table 2 summarizes the therapeutic recommendations for celecoxib, flurbiprofen, ibuprofen, and lornoxicam prescribing based on CYP2C9 phenotype. These NSAIDs exhibit a short to moderately long elimination half-life in CYP2C9 NMs (celecoxib: 11–16 hours; flurbiprofen: 2–6 hours; ibuprofen: 2–4 hours; lornoxicam: 3–5 hours) (26–32). Based on current evidence (Tables S1 to S4), NMs and IMs with an AS of 1.5 are recommended to initiate therapy with the approved starting dose. Despite having mildly reduced metabolism, IMs with an AS of 1.5 do not exhibit significant increases in drug exposure relative to NMs (Figures S2 to S4). While study populations sizes were small, a meta-analysis of five studies showed that the CYP2C9*1/*2 genotype (IM with an AS of 1.5) had no effect on celecoxib exposure (ratio of means 0.98, 95% confidence interval (CI) 0.8 – 1.2 vs. *1/*1) and a meta-analysis of four studies suggested that a potential effect on ibuprofen exposure (ratio of means 1.35, 95% CI 0.9 – 2.0 vs. *1/*1, p=0.09) would be mild if it exists. Given the wide therapeutic index of NSAIDs, dose reductions would not be recommended.

TABLE 2.

THERAPEUTIC RECOMMENDATIONS FOR CELECOXIB, FLURBIPROFEN, LORNOXICAM, AND IBUPROFEN BASED ON CYP2C9 PHENOTYPE

Phenotype	Implication	Therapeutic Recommendation	Classification of Recommendation	Other considerations
CYP2C9 Normal Metabolizer	Normal metabolism	Initiate therapy with recommended starting dose. In accordance with the prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals.	Strong
CYP2C9 Intermediate Metabolizer AS of 1.5	Mildly reduced metabolism	Initiate therapy with recommended starting dose. In accordance with the prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals.	Moderate	IMs might have a higher than normal risk of adverse events especially in individuals with other factors affecting clearance of these drugs such as hepatic impairment or advanced age. Further caution should be taken with ibuprofen use in individuals carrying the CYP2C9^2 allele as it is in linkage disequilibrium with CYP2C8^3 and ibuprofen is also metabolized by CYP2C8.
CYP2C9 Intermediate Metabolizer AS of 1	Moderately reduced metabolism; higher plasma concentrations may increase probability of toxicities	Initiate therapy with lowest recommended starting dose. Titrate dose upward to clinical effect or maximum recommended dose with caution. In accordance with the prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals. Carefully monitor adverse events such as blood pressure and kidney function during course of therapy.	Moderate	IMs might have a higher than normal risk of adverse events especially in individuals with other factors affecting clearance of these drugs such as hepatic impairment or advanced age. Further caution should be taken with ibuprofen use in individuals carrying the CYP2C9^2 allele as it is in linkage disequilibrium with CYP2C8^3 and ibuprofen is also metabolized by CYP2C8.
CYP2C9 Poor Metabolizer	Significantly reduced metabolism and prolonged half-life; higher plasma concentrations may increase probability and/or severity of toxicities	Initiate therapy with 25–50% of the lowest recommended starting dose. Titrate dose upward to clinical effect or 25–50% of the maximum recommended dose with caution. In accordance with the prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals. Upward dose titration should not occur until after steady state is reached (at least 8 days for celecoxib and 5 days for ibuprofen, flurbiprofen and lornoxicam after first dose in PMs). Carefully monitor adverse events such as blood pressure and kidney function during course of therapy. Alternatively, consider an alternate therapy not metabolized by CYP2C9 or not significantly impacted by CYP2C9 genetic variants in vivo.	Moderate	Alternative therapies not primarily metabolized by CYP2C9 include aspirin, ketorolac, naproxen and sulindac. Selection of therapy will depend on individual patient treatment goals and risks for toxicity.
Indeterminate	n/a	No recommendation	No Recommendation	n/a

Open in a new tab

Separate drug-specific recommendation tables are available online (1).

CYP2C9 IMs with an AS of 1 have reduced metabolism and are expected to exhibit a prolonged drug half-life and higher plasma concentrations compared to NMs, which may increase probability of toxicities. A meta-analysis of seven small studies showed a ~60% increase of celecoxib AUC (ratio of means 1.62, 95% CI 1.25 – 2.10 *1/*3 vs. *1/*1, p=0.004), and an analysis of four studies of ibuprofen showed an increase in AUC of ~40% (ratio of means 1.43, 95% CI 1.09 – 1.88 *1/*3 vs. *1/*1, p=0.02). Insufficient data exist for formal meta-analyses of flurbiprofen and lornoxicam, and recommendations are based on evaluating each study individually. For IMs with an AS of 1, it is recommended to initiate NSAID therapy with the lowest recommended starting dose and titrate to clinical effect with close monitoring for adverse events such as elevated blood pressure and kidney dysfunction during course of therapy. Regarding ibuprofen use, it should be taken into consideration that while the CYP2C9*2 allele alone might not cause a clinically relevant reduction in clearance, its strong linkage with the decreased function CYP2C8*3 allele may result in impaired R (−) ibuprofen hydroxylation and increased exposure to the parent drug.

Individuals with a CYP2C9 PM phenotype (AS of 0) are expected to have markedly reduced metabolism and are expected to exhibit a pronounced prolongation of drug half-life and increase in plasma concentrations, which may increase the probability and/or severity of toxicities (19–23). A meta-analysis of seven small studies showed a ~400% increase of celecoxib exposure (ratio of means 4.17, 95% CI 1.85 – 9.37 *3/*3 vs. *1/*1, p=0.005; Figure 1), while insufficient data exist for formal meta-analyses of ibuprofen, flurbiprofen and lornoxicam. In this case, therapeutic recommendations involve dose reduction or alternative therapies, coupled with careful monitoring for adverse events, which are consistent with the U.S. Food and Drug Administration (FDA) recommendations for celecoxib and flurbiprofen. It is recommended to initiate therapy with 25–50% of the lowest recommended starting dose (i.e. 50–75% dose reduction), and careful dose titration to clinical effect. Because drug half-life is significantly prolonged in these patients, upward dose titration should not occur until after steady-state is reached, taking into consideration the PM half-life for each drug; of course, dosing may be stopped or decreased due to toxicity at any time. Treatment with an alternative therapy could also be considered. This could include NSAIDs not primarily metabolized by CYP2C9 (such as aspirin, ketorolac (approved for short term use only), metamizole, naproxen, sulindac, etoricoxib, parecoxib, or valdecoxib), or with pharmacokinetic parameters apparently not impacted by CYP2C9 genetic variants in vivo despite CYP2C9 metabolism in vitro (33)(diclofenac, weak level of evidence, see Table S9). Some of these alternative drugs are not available world-wide (e.g., etoricoxib, metamizole, parecoxib and valdecoxib) because of the elevated cardiovascular risk associated with COX-2-selective NSAIDs, and some have serious adverse events that need to be considered (e.g., diclofenac and liver toxicity, metamizole and agranulocytosis). Therefore, individual NSAIDs are not always therapeutically equivalent and the selection of an alternative agent requires careful consideration of drug properties (e.g. half-life (Table S12), potency, metabolism, COX isoenzyme selectivity, off target effects) that may affect efficacy and safety

Meloxicam.

Table 3 summarizes therapeutic recommendations for meloxicam prescribing based on CYP2C9 phenotype. Meloxicam has a longer half-life (15–20 hours, Table S12) than celecoxib and ibuprofen; thus, impaired meloxicam metabolism is expected to cause sustained elevations in drug exposure. Recommendations for CYP2C9 NMs and IMs with an AS of 1.5 are similar to the short half-life NSAIDs and include initiation of therapy with the standard dose while using the lowest effective dosage for shortest duration capable to achieve treatment goals. For IMs with an AS of 1, reduced metabolism and increased plasma concentrations are expected that may increase probability of toxicities. A meta-analysis of four small studies showed a ~80% increase of meloxicam AUC in IMs with an AS of 1 (ratio of means 1.82, 95% CI 1.32 – 2.52 *1/*3 vs. *1/*1, p=0.0025; Figure 1). The recommendations are to either initiate therapy with 50% of the lowest recommended starting dose or choose an alternative therapy, consistent with the recommendations in PMs for short half-life NSAIDs (Table 2). Upward dose titration should not occur until after steady-state is reached (at least seven days), and careful monitoring is recommended. CYP2C9 PMs should be prescribed an alternative therapy because markedly prolonged half-life is expected (i.e., >100 hours) (34). This provides additional guidance to the FDA label recommendations that recommend a lower starting dose in PMs but does not specify the amount of the dose reduction. Recommended alternative therapies are drugs not metabolized by CYP2C9, or with pharmacokinetic parameters not significantly affected by CYP2C9 genetic variants in vivo (see above). Selection of a NSAID with a short half-life (Table 2) could also be considered.

TABLE 3.

THERAPEUTIC RECOMMENDATIONS FOR MELOXICAM BASED ON CYP2C9 PHENOTYPE

Phenotype	Implication	Therapeutic Recommendation	Classification of Recommendation	Other Considerations
CYP2C9 Normal Metabolizer	Normal metabolism	Initiate therapy with recommended starting dose. In accordance with the prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals.	Strong
CYP2C9 Intermediate Metabolizer AS of 1.5	Mildly reduced metabolism	Initiate therapy with recommended starting dose. In accordance with the meloxicam prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals.	Moderate	IMs might have a higher than normal risk of adverse events especially in individuals with other factors affecting clearance of these drugs such as hepatic impairment or advanced age.
CYP2C9 Intermediate Metabolizer AS of 1	Moderately reduced metabolism; higher plasma concentrations may increase probability of toxicities	Initiate therapy with 50% of the lowest recommended starting dose. Titrate dose upward to clinical effect or 50% of the maximum recommended dose with caution. In accordance with the meloxicam prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals. Upward dose titration should not occur until after steady state is reached (at least 7 days). Carefully monitor adverse events such as blood pressure and kidney function during course of therapy. Alternatively, consider alternative therapy. Choose an alternative therapy not metabolized by CYP2C9 or not significantly impacted by CYP2C9 genetic variants in vivo or choose an NSAID metabolized by CYP2C9 but with a shorter half-life (Table 2).	Moderate	IMs might have a higher than normal risk of adverse events especially in individuals with other factors affecting clearance of these drugs such as hepatic impairment or advanced age. Alternative therapies not primarily metabolized by CYP2C9 include aspirin, ketorolac, naproxen and sulindac. Selection of therapy will depend on individual patient treatment goals and risks for toxicity.
CYP2C9 Poor Metabolizer	Significantly reduced metabolism and prolonged half-life; higher plasma concentrations may increase probability and/or severity of toxicities	Choose an alternative therapy not metabolized by CYP2C9 or not significantly impacted by CYP2C9 genetic variants in vivo or choose an NSAID metabolized by CYP2C9 but with a shorter half-life (Table 2).	Moderate
Indeterminate	n/a	No recommendation	No Recommendation	n/a

Open in a new tab

Separate drug-specific recommendation tables are available online (1).

Piroxicam and tenoxicam.

Table 4 summarizes therapeutic recommendations for piroxicam and tenoxicam. These drugs have extremely long half-lives (30–86 and 60 hours, respectively), thus amplifying the potential risks in individuals with reduced CYP2C9 metabolism and hampering dose titration strategies due to lack of data. Accordingly, rather than use of a lower starting dose, IMs with an AS of 1 and PMs are recommended to receive an alternative therapy. This includes drugs that are not metabolized by CYP2C9 or significantly affected by CYP2C9 genetic variants in vivo. Selection of a NSAID with a short half-life (Table 2) could also be considered.

TABLE 4.

THERAPEUTIC RECOMMENDATIONS FOR PIROXICAM AND TENOXICAM BASED ON CYP2C9 PHENOTYPE

Phenotype	Implication	Therapeutic Recommendation	Classification of Recommendation – Piroxicam	Classification of Recommendation – Tenoxicam	Other Considerations
CYP2C9 Normal Metabolizer	Normal metabolism	Initiate therapy with recommended starting dose. In accordance with the prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals.	Strong	Strong
CYP2C9 Intermediate Metabolizer AS of 1.5	Mildly reduced metabolism	Initiate therapy with recommended starting dose. In accordance with the prescribing information, use the lowest effective dosage for shortest duration consistent with individual patient treatment goals.	Moderate	Moderate	IMs might have a higher than normal risk of adverse events especially in individuals with other factors affecting clearance of these drugs such as hepatic impairment or advanced age.
CYP2C9 Intermediate Metabolizer AS of 1	Moderately reduced metabolism; higher plasma concentrations may increase probability of toxicities	Choose an alternative therapy not metabolized by CYP2C9 or not significantly impacted by CYP2C9 genetic variants in vivo or choose an NSAID metabolized by CYP2C9 but with a shorter half-life (Table 2).	Moderate	Optional	Alternative therapies not primarily metabolized by CYP2C9 include aspirin, ketorolac, naproxen and sulindac. Selection of therapy will depend on individual patient treatment goals and risks for toxicity.
CYP2C9 Poor Metabolizer	Significantly reduced metabolism and prolonged half-life; higher plasma concentrations may increase probability and/or severity of toxicities	Choose an alternative therapy not metabolized by CYP2C9 or not significantly impacted by CYP2C9 genetic variants in vivo or choose an NSAID metabolized by CYP2C9 but with a shorter half-life (Table 2).	Moderate	Optional	Alternative therapies not primarily metabolized by CYP2C9 include aspirin, ketorolac, naproxen and sulindac. Selection of therapy will depend on individual patient treatment goals and risks for toxicity.
Indeterminate	n/a	No recommendation	No Recommendation	No recommendation	n/a

Open in a new tab

Separate drug-specific recommendation tables are available online (1).

Aceclofenac, aspirin, diclofenac, indomethacin, lumiracoxib, metamizole, nabumetone and naproxen.

Table S9 includes evidence linking CYP2C9 genotype to aceclofenac, aspirin, diclofenac, indomethacin, lumiracoxib, metamizole, nabumetone and naproxen phenotype. The pharmacokinetics of these drugs are not significantly impacted by CYP2C9 genetic variants in vivo and/or there is insufficient evidence to provide a recommendation to guide clinical practice at this time (CPIC classification of recommendation “no recommendation”; CPIC level C; Table S2).

Pediatrics.

Data describing the relationship between CYP2C9 genotype and NSAID systemic exposure and toxicities in pediatric patients are scarce (35). Because CYP2C9 activity is fully mature by early childhood, it may be appropriate to extrapolate these recommendations to adolescents or possibly younger children with close monitoring. Ultimately, additional research and clinical trials in pediatric patients investigating the association between CYP2C9 genotype and NSAID systemic exposure and treatment outcomes are needed.

Recommendations for Incidental Findings

See the CPIC guidelines for CYP2C9 and warfarin and phenytoin for genotype-based recommendations for these drugs (4, 8).

Other Considerations

The potential for drug-drug interactions should be considered when initiating NSAID therapy. CYP2C9 decreased function allele carriers are at higher risk of supratherapeutic INR or major bleeding with concomitant use of warfarin or other coumarin anticoagulants with NSAIDs, compared to NMs (36–40). Thus, it is recommended that this drug combination be avoided in CYP2C9 IMs and PMs. Variants in other genes, including CYP2C8 and drug targets such as PTGS1 and PTGS2, may also influence the outcome of NSAID therapy, but the evidence is insufficient to recommend using these variants to guide NSAID dosing at this time (see Supplemental Material).

Implementation of this Guideline:

The guideline supplement and CPIC website (https://cpicpgx.org/cpic-guideline-for-nsaids-based-on-cyp2c9-genotype/) contains resources that can be used within electronic health records (EHRs) to assist clinicians in applying genetic information to patient care for the purpose of drug therapy optimization (see Resources to incorporate pharmacogenetics into an electronic health record with clinical decision support in the Supplemental Material).

POTENTIAL BENEFITS AND RISKS FOR THE PATIENT

The potential benefits for patients with existing CYP2C9 genotyping information are avoiding adverse events in those patients who are CYP2C9 IMs or PMs by making significant reductions in their starting dose or by selecting alternative agents. This may provide an opportunity to prescribe NSAIDs for acute or chronic pain conditions at genetically-informed doses to limit long-term drug exposure and secondary adverse events for patients who may be at increased risk. However, while traditional pharmacogenetics studies have provided substantial evidence associating common CYP2C9 genetic variation with NSAID pharmacokinetics, there is sparse prospective evidence showing that genetically-guided NSAID prescribing improves clinical outcomes. Additionally, study populations were too small to assess interactions between CYP2C9 genetic variation and other factors potentially affecting drug disposition and risk of adverse reactions such as sex, race, ethnicity, age, comorbidities, and concomitant medication. Potential risks associated with CYP2C9 genotyping, which is reliable when performed in qualified laboratories, include errors in genotyping or reporting of genotype.

CAVEATS: APPROPRIATE USE AND/OR POTENTIAL MISUSE OF GENETIC TESTS

Rare CYP2C9 variants may not be included in the genotype test used, and patients with rare variants may be assigned an NM phenotype based on a default CYP2C9*1/*1 test result. Thus, an assigned CYP2C9*1 allele could potentially harbor a decreased or no function variant. Therefore, it is important that genetic test reports include information on which variant alleles were genotyped or which SNPs were interrogated.

As with any diagnostic test, CYP2C9 genotype is just one factor that clinicians should consider when prescribing NSAIDs to an individual patient. Age, sex, race and ethnicity, liver dysfunction, comorbidities, concomitant medications, genetic linkage disequilibrium with CYP2C8, and other undiscovered genetic and environmental factors can all impact the likelihood that a patient will experience adverse events with NSAID therapy. For example, regardless of CYP2C9 phenotype, NSAIDs should be avoided in patients with renal dysfunction or heart failure and in those at high risk of cardiovascular or gastrointestinal adverse events. NSAIDs should be used with caution in elderly patients, as hepatic CYP2C9 metabolism decreases with older age and these individuals are at greater risk of renal and gastrointestinal adverse events. Another consideration is the impact of drug-drug interactions. In particular, concomitant use of NSAIDs and agents with anti-platelet or anticoagulant effects should only be with extreme caution, as this can result in an increased risk of bleeding. NSAIDs decrease the therapeutic effect of anti-hypertensive medications and should be used with caution in patients with underlying hypertension.

Supplementary Material

NIHMS1687646-supplement-Supplementary_Material.docx^{(3.3MB, docx)}

ACKNOWLEDGEMENT

We acknowledge the critical input of Dr. Mary V. Relling (St Jude Children’s Research Hospital) and the members of the Clinical Pharmacogenetics Implementation Consortium (CPIC). This work was funded by the National Institutes of Health (NIH) for CPIC (R24GM115264 and U24HG010135), PharmGKB (R24GM61374) and PharmVar (R24 GM123930).

Funding:

This work was funded by the National Institutes of Health (NIH) for CPIC (R24GM115264 and U24HG010135), PharmGKB (R24GM61374) and PharmVar (R24 GM123930).

Footnotes

DISCLAIMER

Clinical Pharmacogenetics Implementation Consortium (CPIC) guidelines reflect expert consensus based on clinical evidence and peer-reviewed literature available at the time they are written and are intended only to assist clinicians in decision-making, as well as to identify questions for further research. New evidence may have emerged since the time a guideline was submitted for publication. Guidelines are limited in scope and are not applicable to interventions or diseases not specifically identified. Guidelines do not account for all individual variation among patients and cannot be considered inclusive of all proper methods of care or exclusive of other treatments. It remains the responsibility of the health care provider to determine the best course of treatment for the patient. Adherence to any guideline is voluntary, with the ultimate determination regarding its application to be solely made by the clinician and the patient. CPIC assumes no responsibility for any injury to persons or damage to property related to any use of CPIC’s guidelines, or for any errors or omissions.

Conflicts of Interest: All other authors declared no competing interests for this work.

REFERENCES

(1).CPIC. CPIC Guideline for NSAIDs based on on CYP2C9 genotype. <https://cpicpgx.org/cpic-guideline-for-nsaids-based-on-cyp2c9-genotype/>.
(2).PharmGKB. Gene-specific Information Tables for CYP2C9. <https://www.pharmgkb.org/page/cyp2c9RefMaterials>.
(3).Lee CR, Goldstein JA & Pieper JA Cytochrome P450 2C9 polymorphisms: a comprehensive review of the in-vitro and human data. Pharmacogenetics 12, 251–63 (2002). [DOI] [PubMed] [Google Scholar]
(4).Caudle KE et al. Clinical pharmacogenetics implementation consortium guidelines for CYP2C9 and HLA-B genotypes and phenytoin dosing. Clin Pharmacol Ther 96, 542–8 (2014). [DOI] [PMC free article] [PubMed] [Google Scholar]
(5).Vogl S, Lutz RW, Schonfelder G. & Lutz WK CYP2C9 genotype vs. metabolic phenotype for individual drug dosing--a correlation analysis using flurbiprofen as probe drug. PLoS One 10, e0120403 (2015). [DOI] [PMC free article] [PubMed] [Google Scholar]
(6).Kusama M, Maeda K, Chiba K, Aoyama A. & Sugiyama Y. Prediction of the effects of genetic polymorphism on the pharmacokinetics of CYP2C9 substrates from in vitro data. Pharm Res 26, 822–35 (2009). [DOI] [PubMed] [Google Scholar]
(7).Lindh JD, Holm L, Andersson ML & Rane A. Influence of CYP2C9 genotype on warfarin dose requirements--a systematic review and meta-analysis. Eur J Clin Pharmacol 65, 365–75 (2009). [DOI] [PubMed] [Google Scholar]
(8).Johnson JA et al. Clinical Pharmacogenetics Implementation Consortium (CPIC) Guideline for Pharmacogenetics-Guided Warfarin Dosing: 2017 Update. Clin Pharmacol Ther 102, 397–404 (2017). [DOI] [PMC free article] [PubMed] [Google Scholar]
(9).Chaney ME, Piontkivska H. & Tosi AJ Retained duplications and deletions of CYP2C genes among primates. Mol Phylogenet Evol 125, 204–12 (2018). [DOI] [PubMed] [Google Scholar]
(10).Speed WC, Kang SP, Tuck DP, Harris LN & Kidd KK Global variation in CYP2C8-CYP2C9 functional haplotypes. Pharmacogenomics J 9, 283–90 (2009). [DOI] [PMC free article] [PubMed] [Google Scholar]
(11).Grosser T, Theken KN & FitzGerald GA Cyclooxygenase Inhibition: Pain, Inflammation, and the Cardiovascular System. Clin Pharmacol Ther 102, 611–22 (2017). [DOI] [PubMed] [Google Scholar]
(12).Grosser T, Fries S. & FitzGerald GA Biological basis for the cardiovascular consequences of COX-2 inhibition: therapeutic challenges and opportunities. J Clin Invest 116, 4–15 (2006). [DOI] [PMC free article] [PubMed] [Google Scholar]
(13).Zhou Y, Boudreau DM & Freedman AN Trends in the use of aspirin and nonsteroidal anti-inflammatory drugs in the general U.S. population. Pharmacoepidemiol Drug Saf 23, 43–50 (2014). [DOI] [PubMed] [Google Scholar]
(14).Gorski T. et al. Use of NSAIDs in triathletes: prevalence, level of awareness and reasons for use. Br J Sports Med 45, 85–90 (2011). [DOI] [PubMed] [Google Scholar]
(15).Walker LA, Zambraski EJ & Williams RF Widespread Use of Prescription Nonsteroidal Anti-Inflammatory Drugs Among U.S. Army Active Duty Soldiers. Mil Med 182, e1709–e12 (2017). [DOI] [PubMed] [Google Scholar]
(16).Lin JH & Lu AY Inhibition and induction of cytochrome P450 and the clinical implications. Clin Pharmacokinet 35, 361–90 (1998). [DOI] [PubMed] [Google Scholar]
(17).Brownstein JS, Sordo M, Kohane IS & Mandl KD The tell-tale heart: population-based surveillance reveals an association of rofecoxib and celecoxib with myocardial infarction. PLoS One 2, e840 (2007). [DOI] [PMC free article] [PubMed] [Google Scholar]
(18).Grosser T, Yu Y. & Fitzgerald GA Emotion recollected in tranquility: lessons learned from the COX-2 saga. Annu Rev Med 61, 17–33 (2010). [DOI] [PubMed] [Google Scholar]
(19).Bhala N. et al. Vascular and upper gastrointestinal effects of non-steroidal anti-inflammatory drugs: meta-analyses of individual participant data from randomised trials. Lancet 382, 769–79 (2013). [DOI] [PMC free article] [PubMed] [Google Scholar]
(20).Solomon SD et al. Effect of celecoxib on cardiovascular events and blood pressure in two trials for the prevention of colorectal adenomas. Circulation 114, 1028–35 (2006). [DOI] [PubMed] [Google Scholar]
(21).Lanas A. et al. Risk of upper gastrointestinal ulcer bleeding associated with selective cyclo-oxygenase-2 inhibitors, traditional non-aspirin non-steroidal anti-inflammatory drugs, aspirin and combinations. Gut 55, 1731–8 (2006). [DOI] [PMC free article] [PubMed] [Google Scholar]
(22).Castellsague J. et al. Individual NSAIDs and upper gastrointestinal complications: a systematic review and meta-analysis of observational studies (the SOS project). Drug Saf 35, 1127–46 (2012). [DOI] [PMC free article] [PubMed] [Google Scholar]
(23).Huerta C, Castellsague J, Varas-Lorenzo C. & Garcia Rodriguez LA Nonsteroidal anti-inflammatory drugs and risk of ARF in the general population. Am J Kidney Dis 45, 531–9 (2005). [DOI] [PubMed] [Google Scholar]
(24).Schjerning Olsen AM et al. Duration of treatment with nonsteroidal anti-inflammatory drugs and impact on risk of death and recurrent myocardial infarction in patients with prior myocardial infarction: a nationwide cohort study. Circulation 123, 2226–35 (2011). [DOI] [PubMed] [Google Scholar]
(25).Hernandez-Diaz S. & Garcia-Rodriguez LA Epidemiologic assessment of the safety of conventional nonsteroidal anti-inflammatory drugs. Am J Med 110 Suppl 3A, 20S–7S (2001). [DOI] [PubMed] [Google Scholar]
(26).Ochoa D. et al. Effect of gender and CYP2C9 and CYP2C8 polymorphisms on the pharmacokinetics of ibuprofen enantiomers. Pharmacogenomics 16, 939–48 (2015). [DOI] [PubMed] [Google Scholar]
(27).Lee YJ et al. Effects of CYP2C9*1/*3 genotype on the pharmacokinetics of flurbiprofen in Korean subjects. Arch Pharm Res 38, 1232–7 (2015). [DOI] [PubMed] [Google Scholar]
(28).Choi CI, Kim MJ, Jang CG, Park YS, Bae JW & Lee SY Effects of the CYP2C9*1/*13 genotype on the pharmacokinetics of lornoxicam. Basic Clin Pharmacol Toxicol 109, 476–80 (2011). [DOI] [PubMed] [Google Scholar]
(29).Guo Y. et al. Role of CYP2C9 and its variants (CYP2C9*3 and CYP2C9*13) in the metabolism of lornoxicam in humans. Drug Metab Dispos 33, 749–53 (2005). [DOI] [PubMed] [Google Scholar]
(30).Garcia-Martin E, Martinez C, Tabares B, Frias J. & Agundez JA Interindividual variability in ibuprofen pharmacokinetics is related to interaction of cytochrome P450 2C8 and 2C9 amino acid polymorphisms. Clin Pharmacol Ther 76, 119–27 (2004). [DOI] [PubMed] [Google Scholar]
(31).Kirchheiner J, Stormer E, Meisel C, Steinbach N, Roots I. & Brockmoller J. Influence of CYP2C9 genetic polymorphisms on pharmacokinetics of celecoxib and its metabolites. Pharmacogenetics 13, 473–80 (2003). [DOI] [PubMed] [Google Scholar]
(32).Lee CR, Pieper JA, Frye RF, Hinderliter AL, Blaisdell JA & Goldstein JA Differences in flurbiprofen pharmacokinetics between CYP2C9*1/*1, *1/*2, and *1/*3 genotypes. Eur J Clin Pharmacol 58, 791–4 (2003). [DOI] [PubMed] [Google Scholar]
(33).Rodrigues AD Impact of CYP2C9 genotype on pharmacokinetics: are all cyclooxygenase inhibitors the same? Drug Metab Dispos 33, 1567–75 (2005). [DOI] [PubMed] [Google Scholar]
(34).Lee HI et al. Strongly increased exposure of meloxicam in CYP2C9*3/*3 individuals. Pharmacogenet Genomics 24, 113–7 (2014). [DOI] [PubMed] [Google Scholar]
(35).Stempak D, Bukaveckas BL, Linder M, Koren G. & Baruchel S. Cytochrome P450 2C9 genotype: impact on celecoxib safety and pharmacokinetics in a pediatric patient. Clin Pharmacol Ther 78, 309–10 (2005). [DOI] [PubMed] [Google Scholar]
(36).Beinema MJ, de Jong PH, Salden HJ, van Wijnen M, van der Meer J. & Brouwers JR The influence of NSAIDs on coumarin sensitivity in patients with CYP2C9 polymorphism after total hip replacement surgery. Mol Diagn Ther 11, 123–8 (2007). [DOI] [PubMed] [Google Scholar]
(37).Malhi H, Atac B, Daly AK & Gupta S. Warfarin and celecoxib interaction in the setting of cytochrome P450 (CYP2C9) polymorphism with bleeding complication. Postgrad Med J 80, 107–9 (2004). [DOI] [PMC free article] [PubMed] [Google Scholar]
(38).van Dijk KN et al. Potential interaction between acenocoumarol and diclofenac, naproxen and ibuprofen and role of CYP2C9 genotype. Thromb Haemost 91, 95–101 (2004). [DOI] [PubMed] [Google Scholar]
(39).Visser LE et al. Allelic variants of cytochrome P450 2C9 modify the interaction between nonsteroidal anti-inflammatory drugs and coumarin anticoagulants. Clin Pharmacol Ther 77, 479–85 (2005). [DOI] [PubMed] [Google Scholar]
(40).Zarza J. Major bleeding during combined treatment with indomethacin and low doses of acenocoumarol in a homozygous patient for 2C9*3 variant of cytochrome p-450 CYP2C9. Thromb Haemost 90, 161–2 (2003). [PubMed] [Google Scholar]

Associated Data

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

Supplementary Materials

Supplementary Material

NIHMS1687646-supplement-Supplementary_Material.docx^{(3.3MB, docx)}

[R1] (1).CPIC. CPIC Guideline for NSAIDs based on on CYP2C9 genotype. <https://cpicpgx.org/cpic-guideline-for-nsaids-based-on-cyp2c9-genotype/>.

[R2] (2).PharmGKB. Gene-specific Information Tables for CYP2C9. <https://www.pharmgkb.org/page/cyp2c9RefMaterials>.

[R3] (3).Lee CR, Goldstein JA & Pieper JA Cytochrome P450 2C9 polymorphisms: a comprehensive review of the in-vitro and human data. Pharmacogenetics 12, 251–63 (2002). [DOI] [PubMed] [Google Scholar]

[R4] (4).Caudle KE et al. Clinical pharmacogenetics implementation consortium guidelines for CYP2C9 and HLA-B genotypes and phenytoin dosing. Clin Pharmacol Ther 96, 542–8 (2014). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R5] (5).Vogl S, Lutz RW, Schonfelder G. & Lutz WK CYP2C9 genotype vs. metabolic phenotype for individual drug dosing--a correlation analysis using flurbiprofen as probe drug. PLoS One 10, e0120403 (2015). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R6] (6).Kusama M, Maeda K, Chiba K, Aoyama A. & Sugiyama Y. Prediction of the effects of genetic polymorphism on the pharmacokinetics of CYP2C9 substrates from in vitro data. Pharm Res 26, 822–35 (2009). [DOI] [PubMed] [Google Scholar]

[R7] (7).Lindh JD, Holm L, Andersson ML & Rane A. Influence of CYP2C9 genotype on warfarin dose requirements--a systematic review and meta-analysis. Eur J Clin Pharmacol 65, 365–75 (2009). [DOI] [PubMed] [Google Scholar]

[R8] (8).Johnson JA et al. Clinical Pharmacogenetics Implementation Consortium (CPIC) Guideline for Pharmacogenetics-Guided Warfarin Dosing: 2017 Update. Clin Pharmacol Ther 102, 397–404 (2017). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R9] (9).Chaney ME, Piontkivska H. & Tosi AJ Retained duplications and deletions of CYP2C genes among primates. Mol Phylogenet Evol 125, 204–12 (2018). [DOI] [PubMed] [Google Scholar]

[R10] (10).Speed WC, Kang SP, Tuck DP, Harris LN & Kidd KK Global variation in CYP2C8-CYP2C9 functional haplotypes. Pharmacogenomics J 9, 283–90 (2009). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R11] (11).Grosser T, Theken KN & FitzGerald GA Cyclooxygenase Inhibition: Pain, Inflammation, and the Cardiovascular System. Clin Pharmacol Ther 102, 611–22 (2017). [DOI] [PubMed] [Google Scholar]

[R12] (12).Grosser T, Fries S. & FitzGerald GA Biological basis for the cardiovascular consequences of COX-2 inhibition: therapeutic challenges and opportunities. J Clin Invest 116, 4–15 (2006). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R13] (13).Zhou Y, Boudreau DM & Freedman AN Trends in the use of aspirin and nonsteroidal anti-inflammatory drugs in the general U.S. population. Pharmacoepidemiol Drug Saf 23, 43–50 (2014). [DOI] [PubMed] [Google Scholar]

[R14] (14).Gorski T. et al. Use of NSAIDs in triathletes: prevalence, level of awareness and reasons for use. Br J Sports Med 45, 85–90 (2011). [DOI] [PubMed] [Google Scholar]

[R15] (15).Walker LA, Zambraski EJ & Williams RF Widespread Use of Prescription Nonsteroidal Anti-Inflammatory Drugs Among U.S. Army Active Duty Soldiers. Mil Med 182, e1709–e12 (2017). [DOI] [PubMed] [Google Scholar]

[R16] (16).Lin JH & Lu AY Inhibition and induction of cytochrome P450 and the clinical implications. Clin Pharmacokinet 35, 361–90 (1998). [DOI] [PubMed] [Google Scholar]

[R17] (17).Brownstein JS, Sordo M, Kohane IS & Mandl KD The tell-tale heart: population-based surveillance reveals an association of rofecoxib and celecoxib with myocardial infarction. PLoS One 2, e840 (2007). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R18] (18).Grosser T, Yu Y. & Fitzgerald GA Emotion recollected in tranquility: lessons learned from the COX-2 saga. Annu Rev Med 61, 17–33 (2010). [DOI] [PubMed] [Google Scholar]

[R19] (19).Bhala N. et al. Vascular and upper gastrointestinal effects of non-steroidal anti-inflammatory drugs: meta-analyses of individual participant data from randomised trials. Lancet 382, 769–79 (2013). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R20] (20).Solomon SD et al. Effect of celecoxib on cardiovascular events and blood pressure in two trials for the prevention of colorectal adenomas. Circulation 114, 1028–35 (2006). [DOI] [PubMed] [Google Scholar]

[R21] (21).Lanas A. et al. Risk of upper gastrointestinal ulcer bleeding associated with selective cyclo-oxygenase-2 inhibitors, traditional non-aspirin non-steroidal anti-inflammatory drugs, aspirin and combinations. Gut 55, 1731–8 (2006). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R22] (22).Castellsague J. et al. Individual NSAIDs and upper gastrointestinal complications: a systematic review and meta-analysis of observational studies (the SOS project). Drug Saf 35, 1127–46 (2012). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R23] (23).Huerta C, Castellsague J, Varas-Lorenzo C. & Garcia Rodriguez LA Nonsteroidal anti-inflammatory drugs and risk of ARF in the general population. Am J Kidney Dis 45, 531–9 (2005). [DOI] [PubMed] [Google Scholar]

[R24] (24).Schjerning Olsen AM et al. Duration of treatment with nonsteroidal anti-inflammatory drugs and impact on risk of death and recurrent myocardial infarction in patients with prior myocardial infarction: a nationwide cohort study. Circulation 123, 2226–35 (2011). [DOI] [PubMed] [Google Scholar]

[R25] (25).Hernandez-Diaz S. & Garcia-Rodriguez LA Epidemiologic assessment of the safety of conventional nonsteroidal anti-inflammatory drugs. Am J Med 110 Suppl 3A, 20S–7S (2001). [DOI] [PubMed] [Google Scholar]

[R26] (26).Ochoa D. et al. Effect of gender and CYP2C9 and CYP2C8 polymorphisms on the pharmacokinetics of ibuprofen enantiomers. Pharmacogenomics 16, 939–48 (2015). [DOI] [PubMed] [Google Scholar]

[R27] (27).Lee YJ et al. Effects of CYP2C9*1/*3 genotype on the pharmacokinetics of flurbiprofen in Korean subjects. Arch Pharm Res 38, 1232–7 (2015). [DOI] [PubMed] [Google Scholar]

[R28] (28).Choi CI, Kim MJ, Jang CG, Park YS, Bae JW & Lee SY Effects of the CYP2C9*1/*13 genotype on the pharmacokinetics of lornoxicam. Basic Clin Pharmacol Toxicol 109, 476–80 (2011). [DOI] [PubMed] [Google Scholar]

[R29] (29).Guo Y. et al. Role of CYP2C9 and its variants (CYP2C9*3 and CYP2C9*13) in the metabolism of lornoxicam in humans. Drug Metab Dispos 33, 749–53 (2005). [DOI] [PubMed] [Google Scholar]

[R30] (30).Garcia-Martin E, Martinez C, Tabares B, Frias J. & Agundez JA Interindividual variability in ibuprofen pharmacokinetics is related to interaction of cytochrome P450 2C8 and 2C9 amino acid polymorphisms. Clin Pharmacol Ther 76, 119–27 (2004). [DOI] [PubMed] [Google Scholar]

[R31] (31).Kirchheiner J, Stormer E, Meisel C, Steinbach N, Roots I. & Brockmoller J. Influence of CYP2C9 genetic polymorphisms on pharmacokinetics of celecoxib and its metabolites. Pharmacogenetics 13, 473–80 (2003). [DOI] [PubMed] [Google Scholar]

[R32] (32).Lee CR, Pieper JA, Frye RF, Hinderliter AL, Blaisdell JA & Goldstein JA Differences in flurbiprofen pharmacokinetics between CYP2C9*1/*1, *1/*2, and *1/*3 genotypes. Eur J Clin Pharmacol 58, 791–4 (2003). [DOI] [PubMed] [Google Scholar]

[R33] (33).Rodrigues AD Impact of CYP2C9 genotype on pharmacokinetics: are all cyclooxygenase inhibitors the same? Drug Metab Dispos 33, 1567–75 (2005). [DOI] [PubMed] [Google Scholar]

[R34] (34).Lee HI et al. Strongly increased exposure of meloxicam in CYP2C9*3/*3 individuals. Pharmacogenet Genomics 24, 113–7 (2014). [DOI] [PubMed] [Google Scholar]

[R35] (35).Stempak D, Bukaveckas BL, Linder M, Koren G. & Baruchel S. Cytochrome P450 2C9 genotype: impact on celecoxib safety and pharmacokinetics in a pediatric patient. Clin Pharmacol Ther 78, 309–10 (2005). [DOI] [PubMed] [Google Scholar]

[R36] (36).Beinema MJ, de Jong PH, Salden HJ, van Wijnen M, van der Meer J. & Brouwers JR The influence of NSAIDs on coumarin sensitivity in patients with CYP2C9 polymorphism after total hip replacement surgery. Mol Diagn Ther 11, 123–8 (2007). [DOI] [PubMed] [Google Scholar]

[R37] (37).Malhi H, Atac B, Daly AK & Gupta S. Warfarin and celecoxib interaction in the setting of cytochrome P450 (CYP2C9) polymorphism with bleeding complication. Postgrad Med J 80, 107–9 (2004). [DOI] [PMC free article] [PubMed] [Google Scholar]

[R38] (38).van Dijk KN et al. Potential interaction between acenocoumarol and diclofenac, naproxen and ibuprofen and role of CYP2C9 genotype. Thromb Haemost 91, 95–101 (2004). [DOI] [PubMed] [Google Scholar]

[R39] (39).Visser LE et al. Allelic variants of cytochrome P450 2C9 modify the interaction between nonsteroidal anti-inflammatory drugs and coumarin anticoagulants. Clin Pharmacol Ther 77, 479–85 (2005). [DOI] [PubMed] [Google Scholar]

[R40] (40).Zarza J. Major bleeding during combined treatment with indomethacin and low doses of acenocoumarol in a homozygous patient for 2C9*3 variant of cytochrome p-450 CYP2C9. Thromb Haemost 90, 161–2 (2003). [PubMed] [Google Scholar]

PERMALINK

Clinical Pharmacogenetics Implementation Consortium (CPIC) Guideline for CYP2C9 and Nonsteroidal Anti-inflammatory Drugs

Katherine N Theken

Craig R Lee

Li Gong

Kelly E Caudle

Christine M Formea

Andrea Gaedigk

Teri E Klein

José A G Agúndez

Tilo Grosser

Abstract

INTRODUCTION

FOCUSED LITERATURE REVIEW

GENE: CYP2C9

Genetic Test Interpretation

TABLE 1.

Available Genetic Test Options

Incidental Findings

Other Considerations

DRUG: NSAIDs

Background

Linking Genetic Variability to Variability in Drug-related Phenotypes

Figure 1. Meta-analysis of the effect of CYP2C9 variant alleles on NSAID exposure.

Therapeutic Recommendations

Celecoxib, flurbiprofen, ibuprofen, lornoxicam.

TABLE 2.

Meloxicam.

TABLE 3.

Piroxicam and tenoxicam.

TABLE 4.

Aceclofenac, aspirin, diclofenac, indomethacin, lumiracoxib, metamizole, nabumetone and naproxen.

Pediatrics.

Recommendations for Incidental Findings

Other Considerations

Implementation of this Guideline:

POTENTIAL BENEFITS AND RISKS FOR THE PATIENT

CAVEATS: APPROPRIATE USE AND/OR POTENTIAL MISUSE OF GENETIC TESTS

Supplementary Material

ACKNOWLEDGEMENT

Footnotes

REFERENCES

Associated Data

Supplementary Materials

ACTIONS

PERMALINK

RESOURCES

Similar articles

Cited by other articles

Links to NCBI Databases