2.2 Pharmacokinetics

Question 1

What is AD(M)E?

Answer 1

Summary of pharmacokinetics:

Absorption
Distribution
Metabolism (excretion)
Elimination

Question 2

Water v lipid solubility

Answer 2

Water:
~ must be aqueous for absorption, distribution, interation with target, passagein circulation

Lipid:
~cross cell membranes by passive diffusion
~ distribute into fatty tissue
~ easy access to action sites in cells
~easily re-absorbed from kidney

Question 3

What happens to drugs in plasma?

Answer 3

Drugs in plasma available for distribution to sites of action, passage to organs of excretion, metabolism

Question 4

Passage of drugs into/from circulation

Answer 4

Cross the vascular endothelium via gaps between cells packed with matrix of proteins that act to retain molecules of high molecular weight

Question 5

How do drugs pass across cell membranes?

Answer 5

Passive diffusion
Active/facilitated diffusion
~ pinocytosis
~ aqueous pores

Question 6

Factors effecting drug movement

Answer 6

Molecular weight
Lipid solubility
Chemical nature

Question 7

How does molecular weight alter absorption of a drug?

Answer 7

High molecular weight compounds will remain at the site of administration

Question 8

How does lipid solubility alter absorption of a drug?

Answer 8

Lipid soluble drugs can readily cross cell membranes

Question 9

How does chemical properties alter absorption of a drug?

Answer 9

Weak acid/base: partially ionised so unionised fraction readily cross cell membranes

Neutral drugs: readily cross cell membranes

Strong acid/base: 100% ionised - polar molecules do not readily cross cell membranes

Question 10

What is pKA

Answer 10

pH + log (conc. protonated species / conc. non-protonated species)

Question 11

What affects the rate of absorption?

Answer 11

• drug properties
• physiological properties
• drug formulation (e.g. coating)

Question 12

How does pH affect drug absorption?

Answer 12

pH varies at different parts of the body so drug pH effects how well it absorbs:

In plasma:
~ weak base (unionised) readily absorbed
~ weak acid (ionised) less readily absorbed

In acid conditions:
~ weak base (ionised) less readily absorbed
~ weak acid (unionised) readily absorbed

Question 13

How does the area of absorbing surface affect absorption?

Answer 13

surface area
compromised surfaces

Question 14

How does local blood flow effect absorption?

Answer 14

vasoconstriction reduces rate of diffusion of a drug from injection site

Question 15

What is bioavailability?

Answer 15

The fraction of administered dose that reaches the circulation in active form
(expressed as a % of total amount)

Question 16

How can bioavailability be determined?

Answer 16

By measuring the amount of drug in the plasma overtime.

Question 17

What is first pass metabolism?

Answer 17

When the drug is extensively metabolised before it reaches the systemic circulation

Question 18

Explain Cmax and Tmax

Answer 18

Cmax (maximal plasma conc. of a drug) at Tmax (time achieved at)

Question 19

What is volume of distribution?

Answer 19

A measure of volume of fluid required to contain the total amount of drug at plasma conc.

Question 20

How is volume of distribution calculated?

Answer 20

Vd = Q/Cp

Q = Dose (total amount of drug in the body) mg/Kg

Cp = Plasma conc ng/ml

Question 21

Why is Vd important?

Answer 21

predicts if a drug is likely to reach target site at effective concs

Determines loadinh dose necessary to achieve target plasma conc

Question 22

Why might drugs accumulate in target tissues?

Answer 22

High lipid solubility (accumulates in fate)

Ion trapping (pH difference across barriers)

Binding to unrelated site from target

Question 23

How are drugs eliminated?

Answer 23

Drug enters, reaches peak, plasma conc falls

Question 24

Which drugs are eliminated more quickly?

Answer 24

water soluble

lipid soluble (reabsorbed)

Question 25

How are drugs metabolised?

Answer 25

Foreign substance so removed

Converted to water soluble form

Metabolised so biologically inactive

Question 26

Main sites of drug metabolism

Answer 26

Liver, plasma, GIT wall, lung, kidney

Question 27

How are lipid soluble drugs metabolised?

Answer 27

Liver - cross liver membrane to reach microsomal enzymes

Oxidation/reduction
Conjugation

Question 28

What is enterohepatic recycling?

Answer 28

Liver cells transfer drugs to bile, delivers to intestines, conjugated, drug reformed (free drug reabsorbed)

Question 29

What is half life?

Answer 29

Time taken for the conc in plasma to fall by 50%

Question 30

Explain elimination by first order kinetics

Answer 30

Expenontial decrease over time

rate of removal proportional to conc.

elimination pathways not saturated - fixed proportion removed over time

Half life independant on dose

Question 31

Explain elimination by zero order kinetics

Answer 31

Linear decrease in plasma drug conc. over time

Fixed amount of drug removed

Elimination pathways saturated

Half life increases with increase of dose

Question 32

What is the important of half life?

Answer 32

Indicates time to reach steady state of plasma

Time taken for drug to be removed from the body and duration of action

Estimation of appropriate dose intervals

Question 33

What are the 2 ‘groups’ of factors that affect of behaviour of a drug in the body?

Answer 33

Drug / product factors

Animal / human factors

Question 34

What does drug pharmacokinetics depend on? (6)

Answer 34

Lipid and water solubility

Stability

Dose

Plasma protein binding

Chirality

Effect of drugs on liver enzymes

Question 35

What will influence the pharmacokinetics of a drug?

Answer 35

Product formation

pH (renal excretion)

Other drugs being used

Question 36

Effect of drugs on liver enzymes

Answer 36

Enzyme induction caused by repeated administration of drugs

Liver enzyme inhibition

Question 37

Consequences of liver enzyme induction/inhibition (3)

Answer 37

Plasma conc. of the drug

Therapeutic efficacy

Time between doses need changing

Question 38

What does drug formulation effect?

Answer 38

Cmax

Tmax

Time drug remains at therapeutic levels

Question 39

How can food effect Cmax and Tmax?

Answer 39

↓ Cmax, ↑Tmax (Competition for absorption)

↓ Cmax, = Tmax (Reaction with food = excreted with food)

= Cmax, ↑Tmax (Delayed time for absorption)

↓ Cmax, ↑Tmax (Food required for absorption)

Question 40

Explain the effect of pH and renal excretion on the fate of drugs in the body

Answer 40

Acidic urine animals eliminate weakly basic drugs most effectively

Alkaline urine animals eliminate weakly acidic drugs mist effectively

Question 41

Effects of drug interaction (4)

Answer 41

Absorption
Plasma protein binding
Metabolism
Excretion

Question 42

What are the animal/human factors affecting the fate of drugs?

Answer 42

Disease
Age
Species/breed
Feeding schedule
Admin route
Time of day
Physiological state
Gender

Question 43

How does disease effect drug pharmacokinetics?

Answer 43

Changes in ggastric/intestinal motility

Damage to epithelial barrier

Reduced blood flow

Distribution

Inflammatory disease

Metabolism and excretion

Question 44

How does age effect pharmacokinetics?

Answer 44

In neonates:
~reduced renal excretion
~reduced hepatic metabolism
~reduced plasma protein binding
~increased GIT absorption
~increased volume of distribution

In aged animals:
~decline in liver and kidney elimination

Question 45

Define side effects

Answer 45

An unwanted action caused by a drug used at therapeutic dose

Question 46

Define adverse drug reaction

Answer 46

(ADR)
Any unwanted vent associated with the use of a drug at therapeutic doses

Question 47

What is type A ADR?

Answer 47

Augmented - expected but exaggerated response (predictable) dose dependant

Question 48

What is type B ADR?

Answer 48

Bizzare - unexpected/abnormal responses (unpredictable) not dose dependant

Question 49

What is type C ADR?

Answer 49

Chronic - only occurs after prolonged use

Question 50

What is type D ADR?

Answer 50

Delayed - occur at remote time from the treatment

Question 51

What is type E ADR?

Answer 51

End of treatment - occur when drug use is abruptly stopped

Question 52

What is type F ADR?

Answer 52

Failure - expected response is not acheived (rarely due to primary failure of a drug)

Question 53

What is the nocebo effect?

Answer 53

ADR reported isnt actually related to the drug