JoVE Logo
Yazarlar
Bize Ulaşın

Oturum Aç

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

This lesson introduces two critical methods in pharmacokinetics, the Wagner-Nelson and Loo-Riegelman methods, used for estimating the absorption rate constant (ka) for drugs administered via non-intravenous routes. The Wagner-Nelson method relates ka to the plasma concentration derived from the slope of a semilog percent unabsorbed time plot. However, it is limited to drugs with one-compartment kinetics and can be impacted by factors like gastrointestinal motility or enzymatic degradation.

On the other hand, the Loo-Riegelman method estimates ka by comparing plasma concentration-time profiles following different administration routes. It provides more comprehensive data, even for drugs with multicompartment characteristics, and aids in understanding drugs' relative bioavailability and absorption characteristics. Yet, it also has limitations, such as the concentration versus time data requirement for both oral and IV drug administration of the same subject and intra-subject between oral and IV administration studies.

Etiketler

Wagner Nelson MethodLoo Riegelman MethodPharmacokineticsAbsorption Rate ConstantKa EstimationPlasma ConcentrationOne compartment KineticsGastrointestinal MotilityEnzymatic DegradationBioavailabilityMulticompartment CharacteristicsConcentration time Profiles

Bölümden 7:

article

Now Playing

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

Pharmacokinetic Models

399 Görüntüleme Sayısı

article

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

Pharmacokinetic Models

94 Görüntüleme Sayısı

article

7.2 : Model Approaches for Pharmacokinetic Data: Compartment Models

Pharmacokinetic Models

79 Görüntüleme Sayısı

article

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

Pharmacokinetic Models

164 Görüntüleme Sayısı

article

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

Pharmacokinetic Models

213 Görüntüleme Sayısı

article

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

Pharmacokinetic Models

62 Görüntüleme Sayısı

article

7.6 : One-Compartment Model: IV Infusion

Pharmacokinetic Models

165 Görüntüleme Sayısı

article

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

Pharmacokinetic Models

64 Görüntüleme Sayısı

article

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

Pharmacokinetic Models

197 Görüntüleme Sayısı

article

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

Pharmacokinetic Models

142 Görüntüleme Sayısı

article

7.11 : Multicompartment Models: Overview

Pharmacokinetic Models

104 Görüntüleme Sayısı

article

7.12 : Two-Compartment Open Model: Overview

Pharmacokinetic Models

98 Görüntüleme Sayısı

article

7.13 : Two-Compartment Open Model: IV Bolus Administration

Pharmacokinetic Models

407 Görüntüleme Sayısı

article

7.14 : Two-Compartment Open Model: IV Infusion

Pharmacokinetic Models

195 Görüntüleme Sayısı

article

7.15 : Two-Compartment Open Model: Extravascular Administration

Pharmacokinetic Models

157 Görüntüleme Sayısı

See More

JoVE Logo

Gizlilik

Kullanım Şartları

İlkeler

Bize Ulaşın

KÜTÜPHANEYE TAVSİYE ET

JoVE HABER BÜLTENLERİ

Araştırma

Eğitim

Yazarlar

Kütüphaneciler

JoVE Hakkında

Telif Hakkı © 2020 MyJove Corporation. Tüm hakları saklıdır