Tools for optimising pharmacotherapy in psychiatry (therapeutic drug monitoring, molecular brain imaging and pharmacogenetic tests): focus on antidepressants

Eap, Chin B.; Gründer, Gerhard; Baumann, Pierre; Ansermot, Nicolas; Conca, Andreas; Crettol, Séverine; Leon, José de; Howes, Oliver; Kim, E.; Lanzenberger, Rupert; Meyer, Jeffrey H.; Moessner, Rainald; Mulder, Hans; Müller, DJ; Reis, Margareta; Riederer, Peter; Ruhé, Henricus G.; Spigset, Olav; Spina, Edoardo; Stegman, B.; Steimer, Werner; Stingl, Julia; Süzen, Sinan; Uchida, Hiroyuki; Unterecker, Stefan; Vandenberghe, Frederik; Hiemke, Christoph

doi:10.1080/15622975.2021.1878427

Cited by 21 publications

(15 citation statements)

References 526 publications

(572 reference statements)

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“…Lower and upper limit of a reference range, respectively, should derive from well-designed clinical studies that relate measured drug concentrations to treatment response or specific adverse drug reactions. For many psychotropic drugs relationships between target engagement (TE) and drug blood concentrations on the one hand and clinical effects and side effects on the other hand are well-documented (2)(3)(4). TE by the respective drug (usually occupancy of neuroreceptors or transporters) can be quantified using molecular neuroimaging techniques like positron emission tomography (PET) and single photon emission computed tomography (SPECT).…”

Section: Introductionmentioning

confidence: 99%

Therapeutic Reference Ranges for Psychotropic Drugs: A Protocol for Systematic Reviews

et al. 2021

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Background: For many psychotropic drugs, monitoring of drug concentrations in the blood (Therapeutic Drug Monitoring; TDM) has been proven useful to individualize treatments and optimize drug effects. Clinicians hereby compare individual drug concentrations to population-based reference ranges for a titration of prescribed doses. Thus, established reference ranges are pre-requisite for TDM. For psychotropic drugs, guideline-based ranges are mostly expert recommendations derived from a conglomerate of cohort and cross-sectional studies. A systematic approach for identifying therapeutic reference ranges has not been published yet. This paper describes how to search, evaluate and grade the available literature and validate published therapeutic reference ranges for psychotropic drugs.Methods/Results: Following PRISMA guidelines, relevant databases have to be systematically searched using search terms for the specific psychotropic drug, blood concentrations, drug monitoring, positron emission tomography (PET) and single photon emission computed tomography (SPECT). The search should be restricted to humans, and diagnoses should be pre-specified. Therapeutic references ranges will not only base upon studies that report blood concentrations in relation to clinical effects, but will also include implications from neuroimaging studies on target engagement. Furthermore, studies reporting concentrations in representative patient populations are used to support identified ranges. Each range will be assigned a level of underlying evidence according to a systematic grading system.Discussion: Following this protocol allows a comprehensive overview of TDM literature that supports a certain reference range for a psychotropic drug. The assigned level of evidence reflects the validity of a reported range rather than experts' opinions.

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Section: Introductionmentioning

confidence: 99%

Therapeutic Reference Ranges for Psychotropic Drugs: A Protocol for Systematic Reviews

et al. 2021

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“…However, older adults are more at risk for adverse events due to altered pharmacokinetics and—dynamics [ 25 ]. TDM for TCAs is well-established in clinical practice, both for therapeutic effect and toxicity [ 26 – 29 ]. For SSRIs, the clinical use of TDM is less frequently employed, especially in older adults [ 30 ].…”

Section: Discussionmentioning

confidence: 99%

Are higher antidepressant plasma concentrations associated with fall risk in older antidepressant users?

et al. 2023

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Purpose Antidepressants are well-established fall-risk increasing drugs (FRIDs) and therefore falls should be considered an important adverse drug event (ADE) of antidepressants. However, not all antidepressant users experience fall incidents and factors associated with increased fall risk among antidepressant users are incompletely understood. Our objective was to explore whether antidepressant plasma concentrations are associated with falls in older antidepressant users. Methods For this study, we included antidepressant users of the multicenter B-PROOF study. Fall incidents were recorded prospectively using fall calendars. Antidepressant plasma concentrations were analyzed by Liquid chromatography-mass spectrometry (LC–MS) at baseline and at 2 years follow-up. The associations between the observed antidepressant concentration and fall risk were assessed using Cox proportional hazard and logistic regression models and adjusted for potential confounders. Results In total 93 selective serotonin reuptake inhibitor (SSRI) and 41 antidepressant (TCA) users were identified. There was a significant association between baseline TCA plasma concentration and fall risk within users (HR 2.50, 95% CI 1.07–5.87, crude model). In the adjusted model, there were no significant associations between concentrations of SSRIs and fall risk. Conclusion There might be an association between plasma concentrations of TCAs and the risk of falling in older users. However, these results needs to be interpreted with caution considering the small sample size and accompanying limitation of confinement to crude analyses. Therefore, these novel findings need to replicated in a larger cohort, preferably including adjustment for potential confounders and more frequent measures of plasma concentrations is needed.

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“…The phenotypic assessment of metabolic pathways has demonstrated its clinical value [ 25 , 32 , 33 ]. Although it is challenging to make a direct comparison between phenotyping and genotyping regarding clinical outcomes, the high phenoconversion rate [ 34 ] leads us to assert that the phenotypic evaluation of CYP and P-gp activity is a more effective tool than genotyping for personalized medicine [ 35 ]. An extensive literature review allowed us to establish tolerance ranges in order to define phenotypic indices for the drugs used in the Geneva cocktail in clinical practice, and it revealed a greater variability of phenotypic indices in our patients.…”

Section: Discussionmentioning

confidence: 99%

Phenotyping Indices of CYP450 and P-Glycoprotein in Human Volunteers and in Patients Treated with Painkillers or Psychotropic Drugs

et al. 2023

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Drug-metabolizing enzymes and drug transporters are key determinants of drug pharmacokinetics and response. The cocktail-based cytochrome P450 (CYP) and drug transporter phenotyping approach consists in the administration of multiple CYP or transporter-specific probe drugs to determine their activities simultaneously. Several drug cocktails have been developed over the past two decades in order to assess CYP450 activity in human subjects. However, phenotyping indices were mostly established for healthy volunteers. In this study, we first performed a literature review of 27 clinical pharmacokinetic studies using drug phenotypic cocktails in order to determine 95%,95% tolerance intervals of phenotyping indices in healthy volunteers. Then, we applied these phenotypic indices to 46 phenotypic assessments processed in patients having therapeutic issues when treated with painkillers or psychotropic drugs. Patients were given the complete phenotypic cocktail in order to explore the phenotypic activity of CYP1A2, CYP2B6, CYP2C9, CYP2C19, CYP2D6, CYP3A, and P-glycoprotein (P-gp). P-gp activity was evaluated by determining AUC0–6h for plasma concentrations over time of fexofenadine, a well-known substrate of P-gp. CYP metabolic activities were assessed by measuring the CYP-specific metabolite/parent drug probe plasma concentrations, yielding single-point metabolic ratios at 2 h, 3 h, and 6 h or AUC0–6h ratio after oral administration of the cocktail. The amplitude of phenotyping indices observed in our patients was much wider than those observed in the literature for healthy volunteers. Our study helps define the range of phenotyping indices with “normal” activities in human volunteers and allows classification of patients for further clinical studies regarding CYP and P-gp activities.

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Tools for optimising pharmacotherapy in psychiatry (therapeutic drug monitoring, molecular brain imaging and pharmacogenetic tests): focus on antidepressants

Cited by 21 publications

References 526 publications

Therapeutic Reference Ranges for Psychotropic Drugs: A Protocol for Systematic Reviews

Therapeutic Reference Ranges for Psychotropic Drugs: A Protocol for Systematic Reviews

Are higher antidepressant plasma concentrations associated with fall risk in older antidepressant users?

Phenotyping Indices of CYP450 and P-Glycoprotein in Human Volunteers and in Patients Treated with Painkillers or Psychotropic Drugs

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