Pharmacology Flashcards
Who needs monitoring while on a drug?
drug:
- narrow therapeutic window
- benefit = very important (eg. cancer treatment)
- serious drug complications
disease:
- close control required (eg. glucose levels in DM)
patient:
- renal impairment
- poor memory
Define pharmacokinetics
how the body handles a drug
Define pharmacodynamics
drug action in body
What are some clinical reasons for monitoring a drug?
- no-one responds to drug in same way
- prescribing decision guided by monitoring (eg. dose adjustment, stop drug)
- aim = increase benefit and reduce harm
How can you measure the effect of a drug?
signs + symptoms
clinical measurement (BP, HR etc.)
lab/radiological markers (cholesterol, CRP etc.)
directly sample drug conc.
What is TDM?
therapeutic drug monitoring
List 3 scenarios for use of TDM
narrow therapeutic index
loss of control is damaging
levels fluctuate/influenced by many factors (eg. diet, other drugs)
When is TDM mainly used?
antibiotics (gentamicin, vancomycin)
digoxin
antiepileptics
lithium
aminophylline
immunosuppressants (eg. ciclosporin)
What are 3 means of passage of how the drug gets to the target?
Lipid-soluble = passively diffuse through membrane phospholipid bilayer
Drug mimics natural protein = actively transported
Small water-soluble molecules = pass through ion channels
Describe passive diffusion with respect to ionised state of drug
unionised = lipid-soluble = easy passage
ionised = water-soluble = difficult passage
What is the function of the blood brain barrier (BBB)?
brain isolated from peripheral environment
function:
- protect brain from harmful substances
- allow nutrients through
- tight capillary endothelial junctions
- enzyme barriers
major rate-limiting factor for drugs
Describe first order kinetics
(exponential)
most common scenario
rate at which body processes drug is related to concentration
as conc increases, rate of reaction (or breakdown of drug) increases
predictable half life
Describe zero order kinetics
zero order = saturation = rate limited
limited capacity of body to process drug
as dose rises above certain level, metabolic process cannot cope, and saturates
drug level starts smoothly but then suddenly shoots up
dose increase - sudden toxicity
Define bioavailability
proportion of parent drug that passes into systemic circulation after administration
How can you improve bioavailability?
change in formulation:
- eg. enteric-coated tablets
route:
- sublingual GTN - avoids liver metabolism that breaks down oral nitrates
use of inhibitors to stop drug being broken down
