Literature DB >> 10783780

Generalized nonlinear models for pharmacokinetic data.

J K Lindsey1, W D Byrom, J Wang, P Jarvis, B Jones.   

Abstract

Phase I trials to study the pharmacokinetic properties of a new drug generally involve a restricted number of healthy volunteers. Because of the nature of the group involved in such studies, the appropriate distributional assumptions are not always obvious. These model assumptions include the actual distribution but also the ways in which the dispersion of responses is allowed to vary over time and the fact that small concentrations of a substance are not easily detectable and hence are left censored. We propose that a reasonably wide class of generalized nonlinear models allowing for left censoring be considered now that this is feasible with current computer power and sophisticated statistical packages. These modelling strategies are applied to a Phase I study of the drug flosequinan and its metabolite. This drug was developed for the treatment of heart failure. Because the metabolite also exhibits an active pharmacologic effect, study of both the parent drug and the metabolite is of interest.

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Year:  2000        PMID: 10783780     DOI: 10.1111/j.0006-341x.2000.00081.x

Source DB:  PubMed          Journal:  Biometrics        ISSN: 0006-341X            Impact factor:   2.571


  7 in total

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2.  Voxel-wise quantification of myocardial perfusion by cardiac magnetic resonance. Feasibility and methods comparison.

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4.  Effects of tracer arrival time on the accuracy of high-resolution (voxel-wise) myocardial perfusion maps from contrast-enhanced first-pass perfusion magnetic resonance.

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Authors:  Benjamin J Cairns; Andrew R Timms; Vincent A A Jansen; Ian F Connerton; Robert J H Payne
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7.  A strategy for residual error modeling incorporating scedasticity of variance and distribution shape.

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  7 in total

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