An association study of <scp><i>ABCG2</i></scp> rs2231142 on the concentrations of allopurinol and its metabolites

Pilon, Marc-Olivier; Leclair, Grégoire; Oussaïd, Essaïd; St‐Jean, Isabelle; Jutras, Martin; Gaulin, Marie-Josée; Mongrain, Ian; Busseuil, David; Rouleau, Jean L.; Tardif, Jean‐Claude; Dubé, Marie‐Pierre; Denus, Simon de

doi:10.1111/cts.13318

Cited by 13 publications

(32 citation statements)

References 34 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…By extension, these findings suggest that carriers of the T allele, taking the same dose as those without the T allele, would be expected to have increased urate-lowering response, rather than the reduced response noted in other work. 3,[20][21][22][23][24] By contrast, some studies 8,21,25 have not found a relationship between ABCG2 genotype and oxypurinol PKs. The results of our study suggest that the reported association between ABCG2 genotype and allopurinol treatment response is not the result of altered oxypurinol PKs and may reflect alterations in urate disposition.…”

Section: Discussionmentioning

confidence: 95%

The impact of genetic variability in urate transporters on oxypurinol pharmacokinetics

Hishe

Stocker

Stamp

et al. 2022

Clinical Translational Sci

View full text Add to dashboard Cite

The genetic determinants of the allopurinol dose-concentration relationship have not been extensively studied. We aimed to clarify what factors, including genetic variation in urate transporters, influence oxypurinol pharmacokinetics (PKs).A population PK model for oxypurinol was developed with NONMEM (version 7.3). The influence of urate transporter genetic variants for ABCG2 (rs2231142 and rs10011796), SLC2A9/GLUT9 (rs11942223), SLC17A1/NPT1 (rs1183201), SLC22A12/URAT1 (rs3825018), SLC22A11/OAT4 (rs17300741), and ABCC4/ MRP4 (rs4148500), as well as other participant factors on oxypurinol PKs was assessed. Data from 325 people with gout were available. The presence of the T allele for ABCG2 (rs2231142) and SLC17A1/NPT1 (rs1183201) was associated with a 24% and 22% increase in oxypurinol clearance, respectively, in univariate analysis. This effect was not significant in the multivariate analysis. In the final model, oxypurinol PKs were predicted by creatinine clearance, diuretic use, ethnicity, and body weight. We have found that genetic variability in the transporters examined does not appear to influence oxypurinol PKs. Study Highlights WHAT IS THE CURRENT KNOWLEDGE ON THE TOPIC?Current knowledge suggests that ABCG2 (rs2231142) genotype is associated with reduced allopurinol treatment response, however, the association with plasma allopurinol or oxypurinol concentrations is less clear. Other renal and gut transporters involved with urate handling have not been extensively studied for an association with altered oxypurinol pharmacokinetics (PKs). WHAT QUESTION DID THIS STUDY ADDRESS?Are genetic variants of renal and gut transporters involved with urate handling, including ABCG2 (rs2231142), associated with altered oxypurinol PKs? WHAT DOES THIS STUDY ADD TO OUR KNOWLEDGE? The primary finding of this research was that urate transporter genetics did not significantly impact oxypurinol PKs. Whereas ABCG2 (rs2231142) and NPT1 (rs1183201) were associated with increased oxypurinol clearance by 24% and 22%, respectively, in a univariate setting, this effect was not retained in the multivariate How to cite this article: Hishe HZ, Stocker SL, Stamp LK, et al. The impact of genetic variability in urate transporters on oxypurinol pharmacokinetics.

show abstract

Section: Discussionmentioning

confidence: 95%

The impact of genetic variability in urate transporters on oxypurinol pharmacokinetics

Hishe

Stocker

Stamp

et al. 2022

Clinical Translational Sci

View full text Add to dashboard Cite

show abstract

“…The selection of individuals was previously reported 15,16 . Succinctly, the two studies included self‐reported “White” males and females aged ≥18 years.…”

Section: Methodsmentioning

confidence: 99%

Females present higher dose‐adjusted drug concentrations of metoprolol and allopurinol/oxypurinol than males

Hindi

Pilon

Meloche

et al. 2023

Clinical Translational Sci

Self Cite

View full text Add to dashboard Cite

Females present a higher risk of adverse drug reactions. Sex‐related differences in drug concentrations may contribute to these observations but they remain understudied given the underrepresentation of females in clinical trials. The aim of this study was to investigate whether anthropometric and socioeconomic factors and comorbidities could explain sex‐related differences in concentrations and dosing for metoprolol and oxypurinol, the active metabolite of allopurinol. We conducted an analysis of two cross‐sectional studies. Participants were self‐described “White” adults taking metoprolol or allopurinol selected from the Montreal Heart Institute Hospital Cohort. A total of 1007 participants were included in the metoprolol subpopulation and 459 participants in the allopurinol subpopulation; 73% and 86% of the participants from the metoprolol and allopurinol subpopulations were males, respectively. Females presented higher age‐ and dose‐adjusted concentrations of both metoprolol and oxypurinol (both p < 0.03). Accordingly, females presented higher unadjusted and age‐adjusted concentration:dose ratio of both metoprolol and allopurinol/oxypurinol compared to males (all p < 3.0 × 10−4). Sex remained an independent predictor of metoprolol concentrations (p < 0.01), but not of oxypurinol concentrations, after adjusting for other predictors. In addition to sex, age, daily dose, use of moderate to strong CYP2D6 inhibitors, weight, and CYP2D6 genotype‐inferred phenotype were associated with concentrations of metoprolol (all p < 0.01). Daily dose, weight, estimated glomerular filtration rate (eGFR), and employment status were associated with oxypurinol concentrations (all p < 0.01). Females present higher dose‐adjusted concentrations of metoprolol and oxypurinol than males. This suggests the need for sex‐specific dosing requirements for these drugs, although this hypothesis should be validated in prospective studies.

show abstract

“…The effect of the ABCG2 gene polymorphisms on the pharmacokinetics of multiple drugs has been demonstrated [ 345 , 346 ]. Upregulated ABCG2 expression leads to a reduction in the drug plasma concentrations [ 347 , 348 , 349 ], while the downregulation and/or reduced-of-function variations tend to produce higher drug levels [ 345 , 350 , 351 ].…”

Section: Pharmacogenomics Of Transportmentioning

confidence: 99%

“…The T carriers of Q141K were linked to high risk of gout and reduced response to gout treatment by allopurinol [ 359 , 360 ]. However, recent studies have found no association between rs2231142 and oxypurinol, or allopurinol riboside plasma concentrations [ 346 , 361 ]. In other studies, the T carriers not only produced high concentrations of other BCRP substrates such as rosuvastatin and imatinib, but also generated a greater therapeutic effect of the drugs [ 345 , 346 , 362 , 363 , 364 , 365 ].…”

Section: Pharmacogenomics Of Transportmentioning

confidence: 99%

“…However, recent studies have found no association between rs2231142 and oxypurinol, or allopurinol riboside plasma concentrations [ 346 , 361 ]. In other studies, the T carriers not only produced high concentrations of other BCRP substrates such as rosuvastatin and imatinib, but also generated a greater therapeutic effect of the drugs [ 345 , 346 , 362 , 363 , 364 , 365 ]. Moreover, the SNP C421A may influence the susceptibility to cancer development, survival, and treatment outcomes [ 366 , 367 , 368 , 369 ].…”

Section: Pharmacogenomics Of Transportmentioning

confidence: 99%

See 1 more Smart Citation

Cannabis Pharmacogenomics: A Path to Personalized Medicine

Babayeva

Loewy

2023

CIMB

View full text Add to dashboard Cite

Cannabis and related compounds have created significant research interest as a promising therapy in many disorders. However, the individual therapeutic effects of cannabinoids and the incidence of side effects are still difficult to determine. Pharmacogenomics may provide the answers to many questions and concerns regarding the cannabis/cannabinoid treatment and help us to understand the variability in individual responses and associated risks. Pharmacogenomics research has made meaningful progress in identifying genetic variations that play a critical role in interpatient variability in response to cannabis. This review classifies the current knowledge of pharmacogenomics associated with medical marijuana and related compounds and can assist in improving the outcomes of cannabinoid therapy and to minimize the adverse effects of cannabis use. Specific examples of pharmacogenomics informing pharmacotherapy as a path to personalized medicine are discussed.

show abstract

An association study of ABCG2 rs2231142 on the concentrations of allopurinol and its metabolites

Cited by 13 publications

References 34 publications

The impact of genetic variability in urate transporters on oxypurinol pharmacokinetics

The impact of genetic variability in urate transporters on oxypurinol pharmacokinetics

Females present higher dose‐adjusted drug concentrations of metoprolol and allopurinol/oxypurinol than males

Cannabis Pharmacogenomics: A Path to Personalized Medicine

Contact Info

Product

Resources

About