Building a structured model of a complex pharmacokinetic system with time delays

Duriova, M; Dedik, Ladislav; Bălan, Mugur C.

doi:10.1007/bf02458295

Cited by 23 publications

(16 citation statements)

References 5 publications

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“…in the Laplace (s) domain (Yamaoka et al 1978;Ďurišová et al 1995). In the last step the physiologically realistic structures of MRT po and MRT im are determined, using Eqs.…”

Section: Methodsmentioning

confidence: 99%

“…ADME is a well-known acronym in pharmacokinetics (see e.g., Eddershaw et al 2000). A design of an ADME related dynamic system is a simple procedure, it can be performed in the following way: a function approximating a drug input into the body is used as an input to an ADME related dynamic system, and a function approximating a response of the body to the drug input is used as an output of ADME related dynamic system (Ďurišová et al 1995;Dedík and Ďurišová 1996;Ďurišová and Dedík 1997;Tvrdoňová et al 2009). Thereafter, the ADME related dynamic systems are simply called "the dynamic systems".…”

Section: Introductionmentioning

confidence: 99%

“…Therefore, several studies described investigations of the dynamic process associated with drug fate and disposition with the aid of dynamic systems. The investigations were performed in the following way: (a) dynamic systems were defined, (b) optimal circulatory models of the dynamic systems were selected through the Akaike information criterion (Akaike 1974) and (c) parameters of the optimal models were estimated (Ďurišová et al 1995;Ďurišová and Dedík 1997;Dedik et al 2009). …”

Section: Introductionmentioning

confidence: 99%

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A physiological view and structures of mean residence times

Ďurišová¹

2014

gpb

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Abstract. The author's previous theoretical study described the determination of a physiologically realistic structure of a mean residence time of an intravenously administered drug (Ďurišová 2012). This study continues previous work and the aim is to determine physiologically realistic structures of mean residence times of a drug administered either orally (MRT po ) or intramuscularly (MRT im ). The determinations are based on the following assumption: a cardiopulmonary, portal, portal-venous, hepatic-portal subsystem, and a subsystem that mathematically represents non-eliminating tissues can be considered to be most important in terms of their impact on MRT po and MRT im . If drug fate and disposition is a linear process, the used method allows developing mathematical models without any prior knowledge or hypothesis concerning drug fate and disposition. This is a great advantage of the method considered here when compared with compartment methods. The research presented in this study was aimed at contributing to the knowledge base of physiological origins of mean residence times.

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“…in the Laplace (s) domain (Yamaoka et al 1978;Ďurišová et al 1995). In the last step the physiologically realistic structures of MRT po and MRT im are determined, using Eqs.…”

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A physiological view and structures of mean residence times

Ďurišová¹

2014

gpb

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“…(2) The use of the method described previously [4, 7] and a theoretical example in which it was assumed that the drug was administered in an intravenous bolus dose to a hypothetical subject.…”

Section: Methodsmentioning

confidence: 99%

“…(7) The use of the general equation (1), the circulatory model developed, and the method described previously [4] to identify the MRT structure.…”

Section: Methodsmentioning

confidence: 99%

Physiologically Based Structure of Mean Residence Time

Ďurišová

2012

The Scientific World Journal

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A mean residence time (MRT) is an important pharmacokinetic parameter. To the author's knowledge, however, a physiologically based structure of MRT (thereafter MRT structure) has not been published so far. Primarily this is because MRT structures cannot be identified by traditional pharmacokinetic methods used for the determination of MRT. Therefore, tools from the theory of linear dynamic systems were used for the structural identification of MRT in this study. The MRT structure identified is physiologically meaningful. Accordingly, it seems that the MRT structure identified may contribute to already established knowledge about MRT.

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Aminoglycoside antibiotics — two decades of their hplc bioanalysis

Šoltés

1999

Biomed. Chromatogr.

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Building a structured model of a complex pharmacokinetic system with time delays

Cited by 23 publications

References 5 publications

A physiological view and structures of mean residence times

A physiological view and structures of mean residence times

Physiologically Based Structure of Mean Residence Time

Aminoglycoside antibiotics — two decades of their hplc bioanalysis

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