2009
DOI: 10.1007/s10928-009-9142-8
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Selection between Michaelis–Menten and target-mediated drug disposition pharmacokinetic models

Abstract: Target-mediated drug disposition (TMDD) models have been applied to describe the pharmacokinetics of drugs whose distribution and/or clearance are affected by its target due to high binding affinity and limited capacity. The Michaelis–Menten (M–M) model has also been frequently used to describe the pharmacokinetics of such drugs. The purpose of this study is to investigate conditions for equivalence between M–M and TMDD pharmacokinetic models and provide guidelines for selection between these two approaches. T… Show more

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Cited by 77 publications
(86 citation statements)
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“…Similar pharmacokinetic properties were observed for BIIB023 in the previous phase 1 clinical study [14]. Whether the observed nonlinearity in clearance of BIIB023 is due to target-mediated drug disposition could not be confirmed due to insufficient information on the pharmacokinetics of soluble TWEAK and soluble TWEAK: BIIB023 complex [29,30]. The BIIB023 population pharmacokinetic results reported here are consistent with results of the noncompartmental analysis of subjects in study 211HV102 and suggest that no dose adjustments would be required for Chinese or Japanese patients relative to Caucasian patients.…”
Section: Figuresupporting
confidence: 68%
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“…Similar pharmacokinetic properties were observed for BIIB023 in the previous phase 1 clinical study [14]. Whether the observed nonlinearity in clearance of BIIB023 is due to target-mediated drug disposition could not be confirmed due to insufficient information on the pharmacokinetics of soluble TWEAK and soluble TWEAK: BIIB023 complex [29,30]. The BIIB023 population pharmacokinetic results reported here are consistent with results of the noncompartmental analysis of subjects in study 211HV102 and suggest that no dose adjustments would be required for Chinese or Japanese patients relative to Caucasian patients.…”
Section: Figuresupporting
confidence: 68%
“…Baseline assessments were performed prior to dosing on Day 1. Follow-up occurred through the final study visit on Day 71, with assessments on Days 3, 4, 6 (±6 hours), and on Days 8,11,15,22,29,35,43, 57 and 71 (±2 days).…”
Section: Clinical Trial Designmentioning
confidence: 99%
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“…This two-way relationship should ideally be described by a target-mediated drug disposition (TMDD) model, which describes both the pharmacokinetic profile and PK-PD relationship. [23] As discussed above, patient immunization will be responsible for reduced MoAb concentrations. This immunisation is in itself dependent on the concentrations of the therapeutic antibody since, for example, the risk of developing anti-infliximab antibodies has been shown to be higher the lower the infliximab concentrations.…”
Section: Pharmacokineticsmentioning
confidence: 99%
“…Cette relation à double sens doit idéalement être décrite par un modèle de type « élimination liée à la cible » (target-mediated drug disposition ou TMDD), qui permet de décrire de façon conjointe la pharmacocinétique et la relation PK-PD. [23] Comme nous l'avons vu plus haut, l'immunisation des patients va être responsable d'une diminution des concentrations de l'AcMo. Cette immunisation est elle-même dépendante des concentrations de l'anticorps thérapeutique.…”
Section: Pharmacocinétiqueunclassified