Drug interactions & metabolism

Question 1

Name 5 main types of drug interactions

Answer 1

1. Absorption reactions
2. Distribution reactions
3. Metabolism reactions
4. Excretion reactions
5. Pharmacodynamic reactions

Question 2

Give 2 examples of drugs that react with metal ions eg Ca, Mg, Fe

Answer 2

Ciprofloxacin

Tetracyclines (eg Doxycycline)

Question 3

Cholestyramine does what with other drugs in the GIT

Answer 3

Absorbs them so dropping their effectiveness

Question 4

How can you minimised the problem of absorption reactions between diff substances

Answer 4

Give at diff times to avoid interaction

Question 5

How does metclopramide influence the uptake of paracetamol in the drug Paramax

Answer 5

It incr gut motility so incr absorption of paracetamol

Question 6

How do PPIs influence the uptake of acid drugs e.g. Ketoconazole (anti fungal)

Answer 6

By reducing stomach acidity - reduces absorption of weak acids

Question 7

How does rifampicin interact with the transporter P-glycoprotein and what affect does this have on Digoxin absorption

Answer 7

P-glycoprotein reduces Digoxin absorption in gut.

Rifampicin INDUCES P-glycoprotein so will reduce level of Digoxin absorbed even more.

Question 8

What effect does clarithromycin have on CYP450 enzymes. How might this influence the metabolism of statins and what might be the consequence

Answer 8

It is an INHIBITOR - will prevent CYP450 from metabolizing free drug.
Will increase free statin in blood - lead to neuropathy.

Question 9

What effect does rifampicin have on CYP450 enzymes. How might this influence the metabolism of statins and what might be the consequence

Answer 9

It is an INDUCER - will speed up metabolism of free drug.

Will have less statin free in blood (but not clinically shown to be an issue)

Question 10

What drugs reduce kidney perfusion.

How does this affect the levels of renally excreted drugs e.g. methotrexate.

Answer 10

NSAIDs e.g. aspirin, ibuprofen reduce kidney perfusion.

This reduces renal excretion so will get incr in methotrexate = toxicity

Question 11

How do antidiuretics influence the excretion of lithium

Answer 11

Antidiuretics retain Na - Lithium v similar molecule so is also retained. = Lithium toxicity

Question 12

How does urine alkilinisation help in OD of aspirin

Answer 12

Increases the excretion of weak acids e.g. aspirin, methotrexate.

Question 13

Additive pharmacodynamic effects:

What is the possible consequence of adding Beta2 agonist (eg ventolin) and diuretics.

Answer 13

Hypokalaemia

Question 14

Additive pharmacodynamic effects:

What is the possible consequence of adding Alcohol and anti-histamines

Answer 14

Drowsiness

Question 15

Additive pharmacodynamic effects:

What is the possible consequence of adding aminoglycosides & ciclosporin

Answer 15

Renal toxicity

Question 16

Opposing effects:

Why should patients on antihypertensives (eg ACE inhibitors) avoid NSAIDs

Answer 16

NSAIDs cause increased BP

Question 17

Why should patients on warfarin avoid too much green veg

Answer 17

Green veg = vit K, which acts as warfarin antagonist

Question 18

Why should patients taking anti-diabetic drugs be cautious of using corticosteroids

Answer 18

Corticosteroids increase blood glucose

Question 19

Name 7 drugs with a narrow therapeutic window and so are at high risk of drug interactions

Answer 19

1. Warfarin (anti coag)
2. Gentamicin (aminoglycoside antibiotic)
3. Tacrolimus (immuno suppressant - transplants)
4. Lithium - (psych sedation)
5. Digoxin - (slow HR - used in congestive hrt fail)
6. Phenytoin (anti-epileptic)
7. Carbamazepine (anti-epileptic)

Question 20

What does a black dot in the BNF indicate

Answer 20

A significant interaction

Question 21

Name 7 common CYP450 INDUCERS

Answer 21

1. Rifampicin
2. Green veg / broccoli etc. (Vit K)
3. Alchohol
4. Smoking
5. St John’s wort
6. Phenytoin
7. Carbamazepine

Question 22

Name7 common CYP450 inhibitors

Answer 22

1. Grapefruit juice
2. Clarithromycin / erythromycin
3. Metronidazole
4. Cimetidine
5. Miconazole
6. Verapamil
7. Amiodarone

Question 23

What are the main 2 aims of drug metabolism

Answer 23

1. Make drug more hydrophillic - easier to excrete in urine

2. Inactivate drug - reduce free amount in system

Question 24

Main 2 sites & enzymes of drug metabolism

Answer 24

1. Liver - CYP450

2. Gut - Monoamine Oxidase (MAO)

Question 25

Principle of first pass metabolism

Answer 25

Orally consumed drugs enter bloodstream at intestine - enter portal system and liver - metabolised before reach any part of body.

Question 26

3 examples of drugs which will be increased in effect by liver damage due to reduced first pass metabolism

Answer 26

Morphine
Propanolol
Diazepam

Question 27

2 main PHASES of drug metabolism

Answer 27

1. Modification - make lipophilic drugs more water soluble

2. Conjugation - add large molecules to drug to make more water soluble

Question 28

3 types of modification and egs

Answer 28

1. Oxidation - Dopamine to adrenaline by MAO
   - Hypoxanthine - xanthine - uric acid by Xanthine oxidase
2. Reduction - Warfarin by CYP450
3. Hydrolysis - in plasma e.g. Aspirin to Salicylic acid.

Question 29

Example of conjugation with a large molecule to make more water soluble

Answer 29

Aspirin added to GLUCORONIC acid - Glucoronide.

Question 30

What is the basic meaning of First order kinetics

Answer 30

There are still sufficient enzymes avail to metabol drug, so rate of drug metabolism is prop. to rate of drug dose increase.

Question 31

What is basic meaning of Zero order kinetics,(non linear / saturation kinetics) why is it important.

Answer 31

All available enzymes have been saturated so as you increase amount of drug the level of metabolism does not increase any further. - Drugs build up in body this way causing toxicity

Question 32

What is a pro-drug - give an example

Answer 32

An inactive form of a drug which is then metabolized to the active form.
e.g. L-DOPA - Dopamine

Question 33

What reduction in GFR might you expect in 50yr old and 70 yr old respectively

Answer 33

25% and 50% reduction in GFR