Tissue distribution Flashcards

1
Q

How is tissue binding measured?

A

Rarely measured directly – inferred from plasma data

  • Characterised by tissue-to-plasma partition coefficient (Kp)
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2
Q

Role of hepatic uptake and efflux transporters in drug disposition:

A

A. Mediate active uptake of drugs into the hepatocyte
- e.g., uptake of atorvastatin by OATP1B1 transporter
Can result in C liver&raquo_space; C plasma

B. Excretion of drug into the bile – efflux transporters
- e.g. excretion of rosuvastatin by BCRP

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3
Q

Importance of tissue distribution of drugs:

A
  • Binding to tissue components and involvement of transporters (uptake or efflux) determine tissue distribution
  • Knowledge of drug partitioning in certain tissues is important to estimate V in drug development
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4
Q

Kp can be determined:

A
  • in vitro – using tissue homogenate or isolated perfused organs
  • in silico – predictive equations based on physicochemical properties of the drug and tissue composition1
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5
Q

Physiologically-based pharmacokinetic (PBPK) modelling and application

A
  • Mathematical description of ADME processes
  • Whole body represented as a multi-compartment of individual organ compartments
  • Organ compartments connected by blood flows in a physiologically meaningful way
  • Physiological parameters
  • Drug specific parameters
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6
Q

Application of PBPK modelling

A
  • Increasingly used as a decision-making tool at all phases of drug development
  • Implemented in custom built or commercial software platforms
  • Consideration of variability (demographic, physiological and/or genetic variability) - creation of virtual subjects
  • Most commonly used to predict drug-drug interaction risk and to inform adequate design of clinical trials
  • Allows prediction of PK in patients by accounting for known modifications in physiology due to disease
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