The impact of human <i>CES1</i> genetic variation on enzyme activity assessed by ritalinic acid/methylphenidate ratios

Stage, Claus; Dalhoff, Kim; Rasmussen, Henrik Berg; Guski, Louise Schow; Thomsen, Ragnar; Bjerre, Ditte; Ferrero-Miliani, Laura; Madsen, Majbritt Busk; Jürgens, Gesche

doi:10.1111/bcpt.13212

Cited by 16 publications

(23 citation statements)

References 24 publications

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“…For TDM of methylphenidate, sampling of plasma at 1-2 h after immediate release or between 5 and 8 h for extended-release formulations are recommended [19]. Stage et al [30] suggested the ritalinic acid/methylphenidate metabolic ratio based on a singlepoint measurement, 3 h after dose (10 mg, Ritalin®) as a marker of CES1 activity. The time point was chosen because of a high correlation with the corresponding AUC ratios (r ≥ 0.90) from 3 h and onwards.…”

Section: Discussionmentioning

confidence: 99%

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Pharmacokinetics of methylphenidate and ritalinic acid in plasma correlations with exhaled breath and oral fluid in healthy volunteers

Arvidsson

Beck

Ackehed

et al. 2019

Eur J Clin Pharmacol

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Purpose The primary aim of this study was to explore the potential of alternative sampling matrices for methylphenidate by assessing the correlations between dl-threo-methylphenidate and dl-threo-ritalinic acid concentrations in exhaled breath and oral fluid with those in plasma, in repeated samples collected after a single oral dose of methylphenidate. The secondary aim was to study the enantioselective pharmacokinetics of methylphenidate in plasma, with a focus on interindividual variability in the metabolism of methylphenidate to ritalinic acid. Methods Twelve healthy volunteers received a single oral dose of dl-threo-methylphenidate (Ritalin® capsules, 20 mg). Venous blood samples were collected for 24 h, and plasma analyzed for threo-enantiomers of methylphenidate and ritalinic acid with LC-MS/MS. Repeated sampling of exhaled breath, using a particle filter device, and of non-stimulated oral fluid, using a felt pad device, was also performed. Exhaled breath and oral fluid were analyzed with a non-enantioselective LC-MS/MS method for dlthreo-methylphenidate and dl-threo-ritalinic acid. Results In all subjects, d-threo-methylphenidate was detectable in plasma for at least 15 h after the dose with a biphasic profile. lthreo-Methylphenidate was measurable in only five subjects and in most cases in low concentrations. However, one female subject displayed a biphasic concentration-time profile for l-threo-methylphenidate. This subject also had the highest d-threo-methylphenidate AUC (191 ng*h/mL versus 32-119 ng*h/mL in the other subjects). d-threo-Ritalinic acid concentrations were on average 25-fold higher (range 6-126) than the corresponding d-threo-methylphenidate concentrations. Single-time point plasma concentration ratios between d-threo-ritalinic acid and d-threo-methylphenidate 1.5-12 h after dose correlated highly (r = 0.88-0.98) with the d-threo-ritalinic acid AUC/d-threo-methylphenidate AUC ratio. In eleven subjects, dl-threo-methylphenidate in oral fluid mirrored the biphasic profile of methylphenidate (sum of dand l-threo-enantiomers) in plasma, but the concentrations in oral fluid were on average 1.8 times higher than in plasma. dl-threo-Methylphenidate was detected in exhaled breath in all subjects, but there was no consistent concentration-time pattern. Conclusions In some subjects, the pharmacologically less active l-threo-enantiomer may contribute to the total plasma methylphenidate concentrations. Monitoring methylphenidate concentrations without enantiomeric determination carries the risk of missing such subjects, which might affect how the plasma concentrations of methylphenidate are interpreted and used for clinical decision making. The use of exhaled breath and oral fluid to assess medication adherence to MPH in patients with ADHD warrants further studies.

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Section: Discussionmentioning

confidence: 99%

“…Sampling closer to dosing may also be more convenient for the patients. The agreement between the two methods (AUC ratios and single-point measurements of metabolite/parent drug) needs to be further studied to assess which ratios and what timepoints would be most relevant for prediction of CES1 activity [30].…”

Section: Discussionmentioning

confidence: 99%

Pharmacokinetics of methylphenidate and ritalinic acid in plasma correlations with exhaled breath and oral fluid in healthy volunteers

Arvidsson

Beck

Ackehed

et al. 2019

Eur J Clin Pharmacol

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“…In contrast, PMs are more likely to experience improvement in ADHD symptoms, but due to their absence of CYP2D6 metabolic activity, they are at also at increased risk of having side effects from atomoxetine and may therefore require lower doses. From a pharmacodynamic perspective, there are a number of interesting findings warranting further investigation related to dopamine and norepinephrine disposition in the brain (e. g., COMT), as well as the contribution of genetic variability in CES1 (carboxylesterase 1) to methylphenidate metabolism [55]. However, the clinical efficacy and utility of testing for these genes remains unknown.…”

Section: Adhd Medicationsmentioning

confidence: 99%

Review and Consensus on Pharmacogenomic Testing in Psychiatry

et al. 2020

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The implementation of pharmacogenomic (PGx) testing in psychiatry remains modest, in part due to divergent perceptions of the quality and completeness of the evidence base and diverse perspectives on the clinical utility of PGx testing among psychiatrists and other healthcare providers. Recognizing the current lack of consensus within the field, the International Society of Psychiatric Genetics assembled a group of experts to conduct a narrative synthesis of the PGx literature, prescribing guidelines, and product labels related to psychotropic medications as well as the key considerations and limitations related to the use of PGx testing in psychiatry. The group concluded that to inform medication selection and dosing of several commonly-used antidepressant and antipsychotic medications, current published evidence, prescribing guidelines, and product labels support the use of PGx testing for 2 cytochrome P450 genes (CYP2D6, CYP2C19). In addition, the evidence supports testing for human leukocyte antigen genes when using the mood stabilizers carbamazepine (HLA-A and HLA-B), oxcarbazepine (HLA-B), and phenytoin (CYP2C9, HLA-B). For valproate, screening for variants in certain genes (POLG, OTC, CSP1) is recommended when a mitochondrial disorder or a urea cycle disorder is suspected. Although barriers to implementing PGx testing remain to be fully resolved, the current trajectory of discovery and innovation in the field suggests these barriers will be overcome and testing will become an important tool in psychiatry.

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“…Genetic variations in CES1, the gene encoding for the CES1 enzyme in the liver, have been shown to impact the enzyme activity towards different substrates in vitro [ 9 ], which could account for differences in MPH hydrolysis among patients. Nevertheless, very little is known about the stability of the drug and whether this could contribute to its low bioavailability in the gut [ 10 , 11 ]. Only recently, the absorption of MPH was modelled based on physicochemical properties of the drug, formulation-related information, and differences in gut physiology along the gastrointestinal tract [ 12 ].…”

Section: Introductionmentioning

confidence: 99%

Stability of Methylphenidate under Various pH Conditions in the Presence or Absence of Gut Microbiota

Aresti-Sanz

Schwalbe

Pereira³

et al. 2021

Pharmaceuticals

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Methylphenidate is one of the most widely used oral treatments for attention-deficit/hyperactivity disorder (ADHD). The drug is mainly absorbed in the small intestine and has low bioavailability. Accordingly, a high interindividual variability in terms of response to the treatment is known among ADHD patients treated with methylphenidate. Nonetheless, very little is known about the factors that influence the drug’s absorption and bioavailability. Gut microbiota has been shown to reduce the bioavailability of a wide variety of orally administered drugs. Here, we tested the ability of small intestinal bacteria to metabolize methylphenidate. In silico analysis identified several small intestinal bacteria to harbor homologues of the human carboxylesterase 1 enzyme responsible for the hydrolysis of methylphenidate in the liver into the inactive form, ritalinic acid. Despite our initial results hinting towards possible bacterial hydrolysis of the drug, up to 60% of methylphenidate is spontaneously hydrolyzed in the absence of bacteria and this hydrolysis is pH-dependent. Overall, our results indicate that the stability of methylphenidate is compromised under certain pH conditions in the presence or absence of gut microbiota.

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The impact of human CES1 genetic variation on enzyme activity assessed by ritalinic acid/methylphenidate ratios

Cited by 16 publications

References 24 publications

Pharmacokinetics of methylphenidate and ritalinic acid in plasma correlations with exhaled breath and oral fluid in healthy volunteers

Pharmacokinetics of methylphenidate and ritalinic acid in plasma correlations with exhaled breath and oral fluid in healthy volunteers

Review and Consensus on Pharmacogenomic Testing in Psychiatry

Stability of Methylphenidate under Various pH Conditions in the Presence or Absence of Gut Microbiota

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