Autori
Contattaci

Accedi

The one-compartment open model leverages urinary excretion data to estimate renal clearance, which gauges the kidney's capacity to expel a drug. This method offers several benefits, including directly measuring drug elimination and assessing the kidney's contribution to overall drug clearance. However, this approach has limitations. It assumes sole renal excretion of the drug, which is not true for all drugs. Accurate urinary excretion and plasma drug concentration measurement can also be technically challenging.

The elimination rate constant can be determined through the rate constant method and the sigma minus method. Both involve plotting the natural logarithm of the plasma concentration versus time or the difference between plasma concentrations at two time points versus time, with the line slope equating to the elimination rate constant. To ensure validity, urinary excretion data should exhibit a linear relationship between urinary excretion and time, a steady excretion rate, and sufficient data points.

In conclusion, urinary excretion data and determining the elimination rate constant are integral to pharmacokinetic analysis, offering valuable insights into drug elimination and clearance within the body.

Dal capitolo 7:

article

Now Playing

7.10 : One-Compartment Open Model: Urinary Excretion Data and Determination of k

Pharmacokinetic Models

57 Visualizzazioni

article

7.1 : Analysis Methods of Pharmacokinetic Data: Model and Model-Independent Approaches

Pharmacokinetic Models

46 Visualizzazioni

article

7.2 : Model Approaches for Pharmacokinetic Data: Compartment Models

Pharmacokinetic Models

47 Visualizzazioni

article

7.3 : One-Compartment Open Model for IV Bolus Administration: General Considerations

Pharmacokinetic Models

104 Visualizzazioni

article

7.4 : One-Compartment Open Model for IV Bolus Administration: Estimation of Elimination Rate Constant, Half-Life and Volume of Distribution

Pharmacokinetic Models

75 Visualizzazioni

article

7.5 : One-Compartment Open Model for IV Bolus Administration: Estimation of Clearance

Pharmacokinetic Models

33 Visualizzazioni

article

7.6 : One-Compartment Model: IV Infusion

Pharmacokinetic Models

105 Visualizzazioni

article

7.7 : One-Compartment Open Model for Extravascular Administration: Zero-Order Absorption Model

Pharmacokinetic Models

35 Visualizzazioni

article

7.8 : One-Compartment Open Model for Extravascular Administration: First-Order Absorption Model

Pharmacokinetic Models

133 Visualizzazioni

article

7.9 : One-Compartment Open Model: Wagner-Nelson and Loo Riegelman Method for ka Estimation

Pharmacokinetic Models

183 Visualizzazioni

article

7.11 : Multicompartment Models: Overview

Pharmacokinetic Models

50 Visualizzazioni

article

7.12 : Two-Compartment Open Model: Overview

Pharmacokinetic Models

62 Visualizzazioni

article

7.13 : Two-Compartment Open Model: IV Bolus Administration

Pharmacokinetic Models

129 Visualizzazioni

article

7.14 : Two-Compartment Open Model: IV Infusion

Pharmacokinetic Models

131 Visualizzazioni

article

7.15 : Two-Compartment Open Model: Extravascular Administration

Pharmacokinetic Models

93 Visualizzazioni

See More

JoVE Logo

Riservatezza

Condizioni di utilizzo

Politiche

Contattaci

SUGGERISCI JOVE ALLA BIBLIOTECA

Newsletter di JoVE

Ricerca

Didattica

Autori

Personale delle biblioteche

CHI SIAMO

Copyright © 2025 MyJoVE Corporation. Tutti i diritti riservati