From Known Knowns to Known Unknowns: Predicting
            <i>in Vivo</i>
            Drug Metabolites

Pelkonen, Olavi; Tolonen, Ari; Korjamo, Timo; Turpeinen, Miia; Raunio, Hannu

doi:10.4155/bio.09.32

Cited by 24 publications

(13 citation statements)

References 133 publications

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“…The knowledge obtained in in silico metabolism of drugs has not yet been transferred to predict the rate of metabolism in PBPK models of toxicological interest because of the differences in the key CYPs involved in metabolism and physicochemical properties of target compounds. Consequently, predictability of hepatic clearance of toxic compounds is limited, mostly focusing of a chemical class or closely related chemicals (Pelkonen et al, 2009, 2011; Coecke et al, 2013; Bessems et al, 2014). …”

Section: Metabolism As Part Of Admet Prediction Modelsmentioning

confidence: 99%

Modeling of interactions between xenobiotics and cytochrome P450 (CYP) enzymes

et al. 2015

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The adverse effects to humans and environment of only few chemicals are well known. Absorption, distribution, metabolism, and excretion (ADME) are the steps of pharmaco/toxicokinetics that determine the internal dose of chemicals to which the organism is exposed. Of all the xenobiotic-metabolizing enzymes, the cytochrome P450 (CYP) enzymes are the most important due to their abundance and versatility. Reactions catalyzed by CYPs usually turn xenobiotics to harmless and excretable metabolites, but sometimes an innocuous xenobiotic is transformed into a toxic metabolite. Data on ADME and toxicity properties of compounds are increasingly generated using in vitro and modeling (in silico) tools. Both physics-based and empirical modeling approaches are used. Numerous ligand-based and target-based as well as combined modeling methods have been employed to evaluate determinants of CYP ligand binding as well as predicting sites of metabolism and inhibition characteristics of test molecules. In silico prediction of CYP–ligand interactions have made crucial contributions in understanding (1) determinants of CYP ligand binding recognition and affinity; (2) prediction of likely metabolites from substrates; (3) prediction of inhibitors and their inhibition potency. Truly predictive models of toxic outcomes cannot be created without incorporating metabolic characteristics; in silico methods help producing such information and filling gaps in experimentally derived data. Currently modeling methods are not mature enough to replace standard in vitro and in vivo approaches, but they are already used as an important component in risk assessment of drugs and other chemicals.

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Section: Metabolism As Part Of Admet Prediction Modelsmentioning

confidence: 99%

Modeling of interactions between xenobiotics and cytochrome P450 (CYP) enzymes

et al. 2015

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“…While these designs are not yet available, they are technically within reach. Pelkonen et al, 2009) the researcher and analysts, so they will be able to augment each other. As recently explained by Jaworska and Hoffmann (2010) via the concept of Bayesian networks, the structure of the testing strategy matters and will influence the risk assessment process.…”

Section: In Vitro Estimation Of Renal Clearancementioning

confidence: 99%

“…Mass spectrometry, in particular, has proven to be an optimal tool to determine metabolites. As Pelkonen and co-workers state (Pelkonen et al, 2009) "…in silico or in vitro, in conjunction with animal data, provide useful and necessary information, on which to base the first PK studies in humans. The prerequisite is to use appropriate and up-to-date techniques and biological preparations."…”

Section: Possible Strategy To Determine Metabolitesmentioning

confidence: 99%

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A roadmap for the development of alternative (non-animal) methods for systemic toxicity testing

Basketter

Clewell

Kimber

et al. 2012

ALTEX

203

165

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“…Nonetheless, regulatory guidelines exist for the characterization of human metabolites according to whether they are deemed to have been adequately tested during preclinical toxicology [Food and Drug Administration, 2012 (http://www.fda.gov/downloads/Drugs/GuidanceComplianceRegulatoryInformation/Guidances/ UCM079266.pdf); International Conference on Harmonization, 2012 (http://www.ich.org/products/guidelines/multidisciplinary/article/ multidisciplinary-guidelines.html)]. Partially as a consequence of these guidelines, there has been much research into the prediction, detection, and quantification of human circulating metabolites (Anderson et al, 2009;Dalvie et al, 2009;Leclercq et al, 2009;Pelkonen et al, 2009;Lutz et al, 2010;Luffer-Atlas, 2012;Loi et al, 2013). The theoretical basis for predicting metabolite exposure has been discussed by Lutz et al (2010).…”

Section: Discussionmentioning

confidence: 99%

A Pharmacokinetic Modeling Approach to Predict the Contribution of Active Metabolites to Human Efficacious Dose

Martin

Hill

Baker

et al. 2016

Drug Metabolism and Disposition

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A preclinical drug candidate, MRK-1 (Merck candidate drug parent compound), was found to elicit tumor regression in a mouse xenograft model. Analysis of samples from these studies revealed significant levels of two circulating metabolites, whose identities were confirmed by comparison with authentic standards using liquid chromatography-tandem mass spectrometry. These metabolites were found to have an in vitro potency similar to that of MRK-1 against the pharmacological target and were therefore thought to contribute to the observed efficacy. To predict this contribution in humans, a pharmacokinetic (PK) modeling approach was developed. At the mouse efficacious dose, the areas under the plasma concentration time curves (AUCs) of the active metabolites were normalized by their in vitro potency compared with MRK-1. These normalized metabolite AUCs were added to that of MRK-1 to yield a composite efficacious unbound AUC, expressed as "parent drug equivalents," which was used as the target AUC for predictions of the human efficacious dose. In vitro and preclinical PK studies afforded predictions of the PK of MRK-1 and the two active metabolites in human as well as the relative pathway flux to each metabolite. These were used to construct a PK model

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From Known Knowns to Known Unknowns: Predicting in Vivo Drug Metabolites

Cited by 24 publications

References 133 publications

Modeling of interactions between xenobiotics and cytochrome P450 (CYP) enzymes

Modeling of interactions between xenobiotics and cytochrome P450 (CYP) enzymes

A roadmap for the development of alternative (non-animal) methods for systemic toxicity testing

A Pharmacokinetic Modeling Approach to Predict the Contribution of Active Metabolites to Human Efficacious Dose

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