Relevance of <i>CYP2B6</i> and <i>CYP2D6</i> genotypes to methadone pharmacokinetics and response in the OPAL study

Victorri-Vigneau, Caroline; Verstuyft, Céline; Bouquié, Regis; Laforgue, Edouard‐Jules; Hardouin, Jean-Benoît; Leboucher, Juliette; Geay, Bertrand; Dano, C.; Challet-Bouju, Gaëlle; Grall‐Bronnec, Marie

doi:10.1111/bcp.13936

Cited by 17 publications

(9 citation statements)

References 46 publications

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“…Mouly et al, 2015; Victorri‐Vigneau et al, 2019; Crist, Clarke, & Berrettini, 2018; Eap et al, 2002; Fonseca & Torrens, 2018…”

Section: Resultsmentioning

confidence: 99%

“…On the other hand, Methadone, the most anciently prescribed opioid use disorder treatment (Kleber, 2008), is widely affected by variability in the dose required to achieve adequate treatment response, due to a fairly inducible hepatic metabolism but also to several genetic polymorphisms affecting its absorption, blood–brain barrier passage, and hepatic disposition. These complex and interacting phenomena lead to a great importance of associated medical conditions, polypharmacy and individual genetic polymorphisms in the personalized prescription of methadone (for recent examples see (Mouly et al, 2015; Victorri‐Vigneau et al, 2019), for a more general review see (Crist, Clarke, & Berrettini, 2018; Eap et al, 2002; Fonseca & Torrens, 2018)). Of note, specific genetic polymorphisms have also been associated with methadone‐induced side‐effects, such as QT length enlargement measures on ECG (for a recent example see [Zerdazi et al, 2019]).…”

Section: Resultsmentioning

confidence: 99%

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Biomarkers to predict staging and treatment response in opioid dependence: A narrative review

Vorspan

Marie-Claire

Bellivier

et al. 2021

Drug Development Research

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Opioid use disorder is a devastating disorder with a high burden in terms of overdose mortality, with an urgent need for more personalized prevention or therapeutic interventions. For this purpose, the description and validation of biological measures of staging or treatment response is a highly active research field. We conducted a narrative review on the pathophysiology of opioid use disorder to propose staging of the disease and search for research studies proposing or demonstrating the predictive value of biomarkers. We propose a IV stage description of opioid use disorder, from (I) vulnerability stage to (II) disease progression, (III) constituted opioid dependence and were several type of treatments can be applied, to the reach a (IV) modified health state. We classified biomarkers studies according to the stage of the disorder they were intended to predict, and to the three categories of methods they used: anatomical and functional aspects of the brain, genetic/transcriptomic/epigenetic studies, and lastly biomarkers of systemic modifications associated with opioid use disorder, especially regarding the immune system. Most studies predicting Stage III that we reviewed collected data from small samples sizes and were cross‐sectional association studies comparing opioid dependent patients and control groups. Pharmacogenetic biomarkers are proposed to predict treatment response. Future research should now emphasize prospective studies, replication in independent samples, and predictive value calculation of each biomarker. The most promising results are multimodal evaluations to be able to measure the state of the brain reward system in living individuals.

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“…Mouly et al, 2015; Victorri‐Vigneau et al, 2019; Crist, Clarke, & Berrettini, 2018; Eap et al, 2002; Fonseca & Torrens, 2018…”

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Biomarkers to predict staging and treatment response in opioid dependence: A narrative review

Vorspan

Marie-Claire

Bellivier

et al. 2021

Drug Development Research

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“…OPAL (NCT01847729) was an observational, cross-sectional, multicenter study involving 10 centers located in the Western region of France. It combined both a clinical evaluation and a prespecified ancillary pharmacogenetic study (34). OPAL was conducted in accordance with the Good Clinical Practice Guidelines and the Declaration of Helsinki and was approved by the local ethics committee.…”

Section: Methodsmentioning

confidence: 99%

Prevalence of Coaddictions and Rate of Successful Treatment Among a French Sample of Opioid-Dependent Patients With Long-Term Opioid Substitution Therapy: The OPAL Study

Grall‐Bronnec

Laforgue²,

Challet-Bouju

et al. 2019

Front. Psychiatry

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Background: Opioid use disorder (OUD) is a worldwide major health concern due to increased early mortality and morbidity. Opioid substitution therapy (OST) is approved in the context of a global OUD treatment (OUDT), in conjunction with psychosocial interventions. Many factors can explain why unsuccessful treatment rates remain high. While the phenomenon of addiction switching is often proposed, it is not known whether this also includes gambling addiction. The primary objective of the OPAL study was to determine the prevalence of coaddictions, including problem gambling, among patients with OUDT. Secondary objectives were to assess the rate of unsuccessful OUDT and to characterize the associated factors. Methods: For this observational transversal multicenter study, patients with OUDT including OST for at least 6 months were recruited. Clinical assessment was based on a clinically structured interview and a set of self-reported questionnaires. Coaddictions were screened using the Fagerström, the CRAFFT, and the Lie/Bet questionnaires. Unsuccessful OUDT was defined as the persistence of opioid use and/or the worsening of another substance use or gambling practice. After a descriptive analysis, a multivariate analysis was performed to identify the factors associated with unsuccessful OUDT. Results: The sample consisted of 263 patients. Prevalence of coaddictions reached 97% of the sample. Problem gambling was associated with 10% of the patients. OUDT was considered as “unsuccessful” for 60% of the patients. Associated factors included having drug-using friends, psychiatric and professional negative consequences related to opioid use, more than one OST-prescribing physician, and impulsivity, especially high scores for lack of premeditation and sensation seeking. Conclusions: This study provides further evidence of the need to consider coaddictions and the usefulness of global addictive evaluations. Poor prognostic factors must alert the clinician to initiate more sustained care. Further implications are discussed.

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“…In vitro studies demonstrate differential metabolism and clearance of methadone by CYP2B6 variants ranging from CYP2B6 * 4 ≥ CYP2B6 * 1 > CYP2B6 * 5 > CYP2B6 * 9 ≥ CYP2B6 * 6 (Gadel et al, 2015 ). CYP2B6 genotype influences the plasma levels of both enantiomers (Victorri-Vigneau et al, 2019 ). Also, decreased clearance and high plasma concentration of methadone enantiomers was observed in patients with CYP2B6 * 1/ * 6 and CYP2B6 * 6/ * 6 compared to controls (Eap et al, 2007 ; Kharasch et al, 2015 ; Kringen et al, 2017 ; Talal et al, 2020 ).…”

Section: Population Disparity In the Use Of Cyp2b6 Substrates And Consequent Exposure To Substrate-specific Adverse Drug Reaction (Adr)mentioning

confidence: 99%

CYP2B6 Functional Variability in Drug Metabolism and Exposure Across Populations—Implication for Drug Safety, Dosing, and Individualized Therapy

et al. 2021

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Adverse drug reactions (ADRs) are one of the major causes of morbidity and mortality worldwide. It is well-known that individual genetic make-up is one of the causative factors of ADRs. Approximately 14 million single nucleotide polymorphisms (SNPs) are distributed throughout the entire human genome and every patient has a distinct genetic make-up which influences their response to drug therapy. Cytochrome P450 2B6 (CYP2B6) is involved in the metabolism of antiretroviral, antimalarial, anticancer, and antidepressant drugs. These drug classes are commonly in use worldwide and face specific population variability in side effects and dosing. Parts of this variability may be caused by single nucleotide polymorphisms (SNPs) in the CYP2B6 gene that are associated with altered protein expression and catalytic function. Population variability in the CYP2B6 gene leads to changes in drug metabolism which may result in adverse drug reactions or therapeutic failure. So far more than 30 non-synonymous variants in CYP2B6 gene have been reported. The occurrence of these variants show intra and interpopulation variability, thus affecting drug efficacy at individual and population level. Differences in disease conditions and affordability of drug therapy further explain why some individuals or populations are more exposed to CYP2B6 pharmacogenomics associated ADRs than others. Variabilities in drug efficacy associated with the pharmacogenomics of CYP2B6 have been reported in various populations. The aim of this review is to highlight reports from various ethnicities that emphasize on the relationship between CYP2B6 pharmacogenomics variability and the occurrence of adverse drug reactions. In vitro and in vivo studies evaluating the catalytic activity of CYP2B6 variants using various substrates will also be discussed. While implementation of pharmacogenomic testing for personalized drug therapy has made big progress, less data on pharmacogenetics of drug safety has been gained in terms of CYP2B6 substrates. Therefore, reviewing the existing evidence on population variability in CYP2B6 and ADR risk profiles suggests that, in addition to other factors, the knowledge on pharmacogenomics of CYP2B6 in patient treatment may be useful for the development of personalized medicine with regards to genotype-based prescription.

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Relevance of CYP2B6 and CYP2D6 genotypes to methadone pharmacokinetics and response in the OPAL study

Cited by 17 publications

References 46 publications

Biomarkers to predict staging and treatment response in opioid dependence: A narrative review

Biomarkers to predict staging and treatment response in opioid dependence: A narrative review

Prevalence of Coaddictions and Rate of Successful Treatment Among a French Sample of Opioid-Dependent Patients With Long-Term Opioid Substitution Therapy: The OPAL Study

CYP2B6 Functional Variability in Drug Metabolism and Exposure Across Populations—Implication for Drug Safety, Dosing, and Individualized Therapy

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