Warfarin Flashcards
1
Q
Target-specific covalent inhibition
A
- continuum or reversibility (irreversible model)
- turnover of E, I, and complex (PK/PD)
- relative conc of E and I (TTDD)
- genetic polymorphisms (pharmacogenomics)
2
Q
MD
A
1.5-2
3
Q
F
A
> 90
4
Q
Tmax
A
1-2
5
Q
Vd
A
0.08-0.12
6
Q
Protein binding
A
> 99
7
Q
Plasma conc
A
1.5-8
8
Q
Terminal half life
A
S: 24-33
R: 35-58
9
Q
Plasma Cl
A
S: 0.10-1 (more potent than R)
R: 0.07-0.35
10
Q
Target-mediated drug disposition
A
-extensive binding and binding to the target influenced the PK (disposition) of the drug
11
Q
TMDD PK characteristics
A
- nonlinear Vd and Cl
- Steep distributive phase for low doses
- long terminal elimination
- dose proportional on MD
- time-lag to css with low dose IV infusion
12
Q
Multiple dosing
A
- nonlinear PK goes away
- pk becomes more predictable
13
Q
Indirect PD response
A
- zero order production
- first order removal rate constant
- drug acts to inhibit this particular biomarker
- inhibiting a turnover process
- peak response is delayed relative to the peak conc of the drug
- delay in response makes monitoring warfarin difficult (due to indirect effect)
14
Q
Warfarin
A
- low hepatic extraction drug
- S-warfarin metabolized by CYP2C9
- R-warfarin metabolizedc by CYP1A1, 1A2, 2C19, 3A4, catechol-O-methyltransferase and ketoreductases
- Targets VKORC1
- slow onset of action and narrow therapeutic window
- lots of DDI (common:
- INR must be measured (target: 2-3)
- dietary interactions (intake of vitamin K)
15
Q
Genetic based dosing
A
- VKORC1
- CYP2C9
- no difference in genetic based dosing and traditional dosing (INR)
