Video: Clearance dei farmaci epatici: ruolo dei trasportatori

In the liver's bile canaliculi, modification of influx and efflux transporters can influence intrinsic clearance.

Transporters play a major role in moving drugs within liver cells. Elaborate models, such as the biopharmaceutical drug disposition classification system, are essential to relate transporters to drug disposition.

It categorizes drugs into four classes based on solubility and permeability. This system provides insights into elimination routes and effects of transporters following oral and intravenous administration.

For instance, Class 1 drugs are less affected by transporters due to their good absorption, which results from high solubility and permeability.

In contrast, Class 2 drugs are highly affected by efflux transporters due to low solubility and high permeability. It results in limited drug absorption and potential efflux back into the gastrointestinal lumen, lowering plasma drug concentration.

Additionally, efflux transporters in the liver canaliculi pump these drugs into the bile.

In the liver and bile canaliculi, influx and efflux transporters modification can influence intrinsic clearance. Transporters play a significant role in moving drugs within liver cells. Elaborate models, such as the Biopharmaceutical Classification System (BCS), are essential to relate transporters to drug disposition. This system categorizes drugs into four classes based on solubility and permeability, providing insights into elimination routes and the effects of transporters following oral and intravenous administration.

Class I: Drugs with high solubility and high permeability, resulting in efficient absorption and minimal transporter influence (e.g., metoprolol, propranolol, and amoxicillin).
Class II: Drugs with low solubility but high permeability, where efflux transporters can significantly limit absorption and pump drugs into bile (e.g., ezetimibe, ibuprofen, and ketoconazole).
Class III: Drugs with high solubility but low permeability, where uptake transporters may enhance absorption (e.g., cimetidine, cephalexin, and ranitidine).
Class IV: Drugs with low solubility and permeability. They often exhibit poor bioavailability due to dual limitations (e.g., itraconazole, chlorothiazide, and furosemide).

By integrating solubility and permeability, the Biopharmaceutical Classification System highlights how transporters influence drug disposition; for instance, Class II drugs face significant challenges due to efflux into the gastrointestinal lumen and biliary excretion.

Dal capitolo 6:

article

Now Playing

6.25 : Hepatic Drug Clearance: Role of Transporters

Pharmacokinetics: Drug Excretion and Clearance

19 Visualizzazioni

article

6.1 : Drug Elimination: Overview

Pharmacokinetics: Drug Excretion and Clearance

495 Visualizzazioni

article

6.2 : Elimination Kinetics: First-Order and Zero-Order

Pharmacokinetics: Drug Excretion and Clearance

163 Visualizzazioni

article

6.3 : Renal Drug Excretion: Overview

Pharmacokinetics: Drug Excretion and Clearance

56 Visualizzazioni

article

6.4 : Renal Drug Excretion: Glomerular Filtration

Pharmacokinetics: Drug Excretion and Clearance

66 Visualizzazioni

article

6.5 : Renal Drug Excretion: Tubular Reabsorption

Pharmacokinetics: Drug Excretion and Clearance

48 Visualizzazioni

article

6.6 : Renal Drug Excretion: Tubular Secretion

Pharmacokinetics: Drug Excretion and Clearance

62 Visualizzazioni

article

6.7 : Renal Drug Excretion: Effect of Urine pH, Flow Rate, and Drug pKa

Pharmacokinetics: Drug Excretion and Clearance

71 Visualizzazioni

article

6.8 : Hepatic Drug Excretion: Enterohepatic Cycling

Pharmacokinetics: Drug Excretion and Clearance

464 Visualizzazioni

article

6.9 : Hepatic Drug Excretion: Influencing Factors

Pharmacokinetics: Drug Excretion and Clearance

43 Visualizzazioni

article

6.10 : Drug Excretion: Pulmonary and Glandular Routes

Pharmacokinetics: Drug Excretion and Clearance

26 Visualizzazioni

article

6.11 : Drug Excretion: Miscellaneous Routes

Pharmacokinetics: Drug Excretion and Clearance

15 Visualizzazioni

article

6.12 : Drug Clearance: Overview

Pharmacokinetics: Drug Excretion and Clearance

29 Visualizzazioni

article

6.13 : Clearance Models: Physiological Models

Pharmacokinetics: Drug Excretion and Clearance

36 Visualizzazioni

article

6.14 : Clearance Models: Compartment Models

Pharmacokinetics: Drug Excretion and Clearance

32 Visualizzazioni

See More

Copyright © 2025 MyJoVE Corporation. Tutti i diritti riservati