NSAIDs

Question 1

What are the properties of NSAIDs?

Answer 1

• analgesic
• anti-pyretic
• anti-inflammatory

Question 2

When are NSAIDs used for their analgesic properties?

Answer 2

• toothache
• headache
• backache
• post-operative
• dysmenorrhoea (menstrual pain)

Question 3

When are NSAIDs used for their anti-pyretic properties?

Answer 3

reducing fever in influenza for example

Question 4

When are NSAIDs used for their anti-inflammatory properties?

Answer 4

• rheumatoid arthritis
• osteoarthritis
• musculoskeletal inflammation
• soft tissue injuries
• gout

Question 5

How do NSAIDs work?

Answer 5

They inhibit the production of prostanoids by COX enzymes (COX1, COX2). COX is the rate limiting step for the production of all prostanoids

Question 6

What are prostonoids?

Answer 6

prostaglandins, thromboxane and prostacyclin

Question 7

What are some features of prostanoids?

Answer 7

• they are widely distributed
• not stored pre-formed, when made they are released
• act on receptors

Question 8

What are all prostanoids made from?

Answer 8

From arachidonic acid

Question 9

Give some examples of prostanoids

Answer 9

PGE2 
PGI2 (prostacyclin)
PGD2
PGF2
Thromboxane

Question 10

How many prostanoid receptors are there?

Answer 10

10 - named based on agonist potency

DP1, DP2, EP1, EP2, EP3, EP4, FP, IP1, IP2, TP

Question 11

Are prostanoid receptors specific?

Answer 11

NO - different prostanoids can act on the same receptor hence the effects of inhibiting prostanoid production can have multiple complex effects

Question 12

How do prostanoid receptors work?

Answer 12

They have G protein dependent and independent actions

Question 13

Which receptors does PGE2 activate?

What are the unwanted effects of PGE2?

Answer 13

PGE2 can activate 4 different receptors (EP1, EP2, EP3 and EP4)

Unwanted effects of PGE2:

• Increased pain perception
• Increased body temperature
• Acute inflammatory response
• Immune responses
• Tumorigenesis
• Inhibition of apoptosis

Question 14

What do PGE2 analogues do?

Answer 14

• They lower the pain threshold (nociceptors cause pain, both acutely and chronically)
• Stimulation of PG receptors in the periphery sensitises nociceptors -> lowers pain threshold
• Co-injection of a COX 2 inhibitor prevents or reduces the duration of prolonged pain

Question 15

How do prostanoids lower the pain threshold?

Answer 15

Mechanisms are unclear

• EP1 receptors and EP4 receptors (EP4 in periphery and spine)
• Endocannabinoids (neuromodulators in thalamus, spine and periphery)
• Increasing beta-endorphin in spine
• Not mutually exclusive

Question 16

How is PGE2 pyrogenic?

Answer 16

• It stimulates hypothalamic neurones initiating a rise in body temperature
• Animals were treated with lipopolysaccharide (found on gram –ve bacteria, highly pro-inflammatory)
• Once injected, the levels of PGE2 raised dramatically, followed by dramatic increase in temperature

Question 17

How is PGE2 involved in inflammation?

Answer 17

• The role of PGE2-EP3 signalling in acute inflammation EP3 works through multiple mechanisms - calcium regulated and through G protein coupled receptors.
• There is cross-talk between cells
• Keratinocytes are stimulated by external stimuli to produce PGE2
• EP3 receptors on mast cells are in turn stimulated
• This produces calcium release -> degranulation -> histamine

Question 18

What are some desirable effects of prostanoids?

Answer 18

• Bronchodilation (except PGD2 which does opposite)
• Renal salt and water homeostasis
• Gastro-protection
• Vaso-regulation (dilation and constriction depending on receptor activated)

Question 19

Why do prostanoids cause bronchodilation?

Answer 19

• Cyclooxygenase inhibition favours production of leukotrienes (bronchoconstrictors
• NSAIDS should not be taken by asthmatic patient

Question 20

How does PGE2 affect the kidney?

Answer 20

Both COX isoforms (COX 1 and 2) are involved at multiple points in the nephron. PGE2 has a role in renal blood flow (increases flow)

Question 21

How can NSAIDs cause renal toxicity?

Answer 21

• Constriction of afferent renal arteriole
• Reduction in renal artery flow
• Reduced glomerular filtration rate

Question 22

What is the role of PGE2 in gastric protection?

Which COX is involved?

Answer 22

• Parietal cells normally produce HCl, secreting it into the stomach hence cells lining stomach must be protected
• They produce a mucous layer and also protect themselves by bicarbonate secretion
• PGE2 normally down-regulates HCl secretion and stimulates mucus and bicarbonate secretion
• THESE ARE BOTH COX 1 DEPENDENT ACTIONS

Question 23

How can NSAIDs have unwanted effects on the stomach and duodenum?

Answer 23

• NSAIDs increase risk of gastric and duodenal ulceration (around 1000 deaths annually in England)
• NSAIDs are taken orally, so there is a high load in the stomach

Question 24

COX1 and COX2 - are they completely isolated in distribution?

Answer 24

• COX-1 and COX-2 have different (but frequently overlapping) cellular distributions

Question 25

Give an example of an NSAID that inhibits COX 1+2 and one that inhibits only COX2

Answer 25

• Both: ibuprofen

- COX2: celecoxib

Question 26

What are COXib drugs?

Answer 26

selectively inhibit COX2: thought to be gastroprotective and even though they were, there were other effect from them

Question 27

What are some serious unwanted CV effects of NSAIDs?

Answer 27

• Vasoconstriction
• Salt and water retention
• Reduce the effects of antihypertensive drugs

Question 28

What CV conditions do NSAIDs have a risk of increasing?

Answer 28

• Hypertension
• Myocardial infarction
• Stroke

Question 29

COX2 inhibitors and CVS effects

Answer 29

• There is increasing evidence that selective COX-2 inhibitors pose higher risk of cardiovascular disease than conventional NSAIDS even though mechanism is unclear
• All the prostanoids have some actions on vasoconstriction or vasodilation – so they all affect the vasculature or platelet aggregation
• If we look specifically at COX-2 (found in the vascular endothelial and smooth muscle cells, the heart and the kidney), there are complex effects. When these are blocked, many unwanted CVS actions may result

Question 30

Give an example of an NSAID that is COX-1 selective?

Answer 30

piroxicam

Question 31

What do all NSAIDs increase the risk of?

Particularly what do COX-2 and COX-1 selective NSAIDs increase the risk of?

Answer 31

• All NSAIDS increase risk of GI bleeds and CVS events
• The more selective the drugs are for COX-1, the more likely you are to get a GI bleed
• The more selective the drugs for COX-2, the more likely you are to have a cardiovascular event

Question 32

What are the risks and benefits of using NSAIDs for analgesic and anti-inflammatory purposes?

Answer 32

• Analgesic use: Usually occasional and relatively low risk of side effects
• Anti-inflammatory use: Often sustained, higher doses and relatively high risk of side effects

Question 33

How can the GI side effects of NSAIDs be avoided? (other than use COX2 selective drugs)

Answer 33

• Topical application
• Minimise NSAID use in patients with history of GI ulceration
• Treat H pylori if present
• If NSAID is essential, administer with omeprazole or other proton pump inhibitor
• Minimise NSAID use in patients with other risk factors and reduce risk factors where possible e.g.
  alcohol consumption, anticoagulant or glucocorticoid steroid use

Question 34

Why is aspirin a unique NSAID?

Answer 34

Binds IRREVERSIBLY to COX enzymes

Question 35

What is aspirin selective for/

Answer 35

COX1 particularly but works by acetylation of both enzyme’s active sites

Question 36

What are the roles of aspirin?

Answer 36

• Has anti-inflammatory, analgesic and anti-pyretic actions

- Reduces platelet aggregatio

Question 37

Why are the effects of aspirin dose dependent?

Answer 37

• Platelets produce thromboxane, which enhances platelet action (pro-aggregatory)
• Endothelial cells produce prostacyclin (PGI2), which decreases platelet action (anti-aggregatory)
• Thromboxane A2 is made by COX-1 in the platelet
• In the endothelial cell is both COX-1 and COX-2 – so PGI2 is reduced, but not totally
• Giving aspirin at a high dose will inhibit thromboxane production
• But it will also reduce prostacyclin production

Question 38

What happens with high and low dose aspirin?

Answer 38

LOW DOSE ASPIRIN: The nucleus in the endothelial cell simply replenishes COX enzymes. However, platelets do not have a nucleus. Therefore they cannot recover to produce more thromboxane after aspirin. This leads to no resynthesis of COX-1 in platelets -> overall reduced platelet aggregation

HIGH DOSE ASPIRIN: There is barely any action on platelet aggregation – this is because endothelial cell COX enzymes will be in a permanent state of inhibition

Question 39

Why does aspirin have anti-platelet activity?

Answer 39

• Very high degree of COX-1 inhibition which effectively suppresses TxA2 production by platelets
• Covalent binding which permanently inhibits platelet COX-1
• Relatively low capacity to inhibit COX-2
• Use low dose to allow endothelial re-synthesis of COX-2

Question 40

What are the side effects of aspirin?

Answer 40

• Gastric irritation and ulceration
• Bronchospasm in sensitive asthmatics
• Prolonged bleeding times
• Nephrotoxicity
• Side effects likely with aspirin because it inhibits COX covalently, not because it is selective for COX-1

Question 41

What is paracetamol used for? Is it an NSAID and why?

Answer 41

• Is a good analgesic for mild-to-moderate pain
• Has anti-pyretic action
• Does not have any anti-inflammatory effect so not an NSAID

Question 42

How does paracetamol work?

Answer 42

• The mechanism of action for paracetamol is not well understood
• Probably central and peripheral mechanism
• Cannabinoid receptors? Endogenous opioids interaction? 5HT and adenosine receptor interaction?

Question 43

Why does paracetamol overdoes cause liver failure?

Answer 43

• Paracetamol is normally metabolised by the cytochrome P450 complex
• A toxic metabolite is produced (NAPQI), which is highly reactive
• At a therapeutic dose, NAPQI is produced is very small amounts and will be mopped up by glutathione (Glutathion-s-transferase)
• If glutathione is depleted the metabolite oxidises thiol groups of key hepatic enzymes and causes cell death

Question 44

What is the antidote for paracetamol poisoning?

Answer 44

• Add compound with –SH groups (usually intravenous acetylcysteine, occasionally oral methionine)
• Acetyl cysteine used in cases of attempted suicide and accidental poisoning
• If not administered early enough, liver failure may be unpreventable

Question 45

How have rules been put in place to reduce paracetamol overdoses?

Answer 45

1998 pack size of paracetamol restricted to 16 x 500 mg tablets per pack

2009 guidelines:

• No more than 2 packs per transaction
• Illegal to sell more than 100 paracetamol in one transaction

Question 46

Has legislation reduced deaths from paracetamol overdose?

Answer 46

Since 2009, deaths from paracetamol overdose have fallen by 43% (~70 people a year) and about 60% fewer registrations for liver transplants (~40 people a year)