NSAIDs

Question 1

What are the drug classes for treatment for RA?

Answer 1

• NSAIDs
• DMARDs
• Biological Agents

Note that both classical and biological DMARDs possess the ability to slow progression of the disease process, an attribute that is not evident with NSAIDs.

Question 2

Is acetaminophen (tylenol) used for RA?

Answer 2

No, even though it is an NSAID, it provides no anti-inflammatory
action (only relief of pain and fever)

Doesn’t change course of disease

Question 3

What NSAIDs can be used for RA?

Answer 3

• Aspirin (acetyl-salicyclic acid)
• Ibuprofen (Motrin, Advil)
• Celecoxib (Celebrex)
• Naproxen, Ketoprofen, Piroxicam

Question 4

What is unique about Celecoxib?

Answer 4

Cox-2 specific drug

Question 5

T or F. NSAID action on COX is reversible

Answer 5

T, except in aspirin

Question 6

What is different between expression of COX-1 and COX-2?

Answer 6

COX-1 is constitutive and COX-2 is inducible

Question 7

How are most NSAIDs metabolized?

Answer 7

extensive hepatic metabolism with predominant elimination in the urine and some in feces

Question 8

What NSAID is noticably metabolized differently?

Answer 8

Ketorolac (58% unchanged in urine) and little in feces

Question 9

What prostaglandin in particular is involved in activation of inflammatory cells?

Answer 9

PGE2.

Question 10

What happens following tissue damage?

Answer 10

mast cells and macrophages are activated and some blood-borne immune cells, including neutrophils may be recruited. Various immune mediators, such as TNF-a, IL-1B, IL-6, and others are released which exert their allegoric effects by a ting directly on nociceptors or indirectly through the release of prostanoids

Question 11

What are the effects of COX-2 inhibition?

Answer 11

• anti-inflammatory
• analgesic
• antipyretic
• increased BP
• reduced urinary PGI2 metabolites

thus, these effects are seen in ALL NSAIDs

Question 12

What are the effects of COX-1 inhibition?

Answer 12

• reduce urinary TXA2

- inhibit platelet activity and increase bleeding time

Question 13

GI toxicity is related to inhibition of which COX enzyme?

Answer 13

possibly both

Question 14

What ‘traditional’ NSAIDs have a propensity for COX-2 over COX-1?

Answer 14

etodolac

Question 15

What ‘traditional’ NSAIDs have a propensity for COX-1 over COX-2?

Answer 15

ketorolac

Question 16

How does chronic NSAID consumption lead to gastric damage and bleeding?

Answer 16

Not only is there direct chemical irritation of the mucosal tissue but the inhibition of PGE2 interrupts essential cytoprotective mechanisms in the stomach involving mucus secretion, bicarbonate release and the initiation of essential repair processes in underlying tissue.

Question 17

What are some risk factors for GI bleeding with NSAIDs?

Answer 17

• older age (risk doubles ever decade over 55)
• male sex
• CV disease, HTN, diabetes, hepatic or renal impairment

Question 18

Other risk factors for GI bleeding with NSAIDs?

Answer 18

• helicobacter pylori infection
• excessive alcohol use
• heavy smoking

Question 19

What concurrent meds can increase risk of GI bleed with NSAIDs?

Answer 19

• aspirin
• warfarin
• oral corticosteroids
• SSRIs
• venlafaxine or duloxetine

Question 20

What are some ways to reduce GI bleed risk with NSAIDs?

Answer 20

• enteric coating (doesn’t eliminate)
• MAYBE advocate taking NSAIDs on an empty stomach to achieve faster onset of action and avoid ‘extra’ doses because relief isn’t met fast enough by the patient

Question 21

Other ways to reduce GI bleed risk with NSAIDs?

Answer 21

-COX-2
-co-administer prostaglandin analogue misoprostol, or more usually these days an H2 receptor antagonist or proton pump inhibitor.
-

Question 22

What is the benefit of PPIs with NSAIDs?

Answer 22

possesses superior effectiveness due to the more complete suppression of acid
secretion, a mechanism-based issue (just as good as a COX-2)

Question 23

What should be considered when giving a PPI with an NSAID?

Answer 23

-PPIs can alter the efficacy of concurrent drugs that rely on stomach acidity for absorption

Question 24

Contraindications of PPIs?

Answer 24

concurrent with cloidogrel

Question 25

What NSAID will not change the balance between TXA2 and PGI2, and thus lower CV exacerbation risk?

Answer 25

ibuprofen because it doesn’t have an increased affinity for COX-1 or COX-2

Question 26

What is another potential thing to consider with a COX-2 inhibitor?

Answer 26

promotes shift toward TXA2 production from COX-1 and thus a pro-thrombotic state

Question 27

T or F. High doses of ibuprofen is associated with increased risk of vascular events

Answer 27

T. Even though it is COX neutral.

Question 28

High dose of what NSAID is not associated with increased CV related (thrombo-forming) risk?

Answer 28

Naproxen

Question 29

What is the major difference between NSAIDs and aspirin?

Answer 29

aspirin irreversibly inhibits the COX enzyme by acetylating it.

Question 30

DD interaction of aspirin?

Answer 30

There is a real potential for concurrent administration of NSAIDs to inhibit the ability of low-dose aspirin to reach its binding site in the platelet and to provide irreversible enzyme inhibition in prophylaxis of MI.

Since the traditional NSAID action is reversible, there is a potential for antiplatelet activity to be lost and increased cardiovascular risk to occur.

Question 31

Which NSAID has the highest risk of hepatotoxicity?

Answer 31

Sulindac (via hypersensitivity mechanism)

Question 32

What is the role of PGE2 and PGI2 at the kidneys?

Answer 32

Prostaglandin I2 and E2 play an important role in micro-regulation of perfusion in renal tissue, most especially in abnormal “stress” situations where they help to maintain GFR.

and NSAIDS can block this!!*

Question 33

What is the effect of chronic NSAID use by blocking PGE2 and PGI2?

Answer 33

reversible renal ischemia, reduced glomerular hydraulic pressure and reduced GFR

Question 34

NSAIDs decrease the clearance of what drugs?

Answer 34

lithium and methotrexate

Question 35

T or F. NSAIDs can
antagonize the effects of
uricosuric agents.

Answer 35

T.

Question 36

Recommended patient monitoring with chronic NSAID use

Answer 36

• LFTs
• Serum creatinine/BUN
• Stool guaiac
• CBC

Question 37

Why get CBC with chronic NSAID use?

Answer 37

NSAIDs can rarely cause various blood dyscrasia

Question 38

Chronic aspirin therapy may warrant monitoring of _______

Answer 38

serum salicylate

Question 39

What does overdose of salicylate cause?

Answer 39

capable of passing across the BBB where it stimulates the respiratory centre, resulting in respiratory alkalosis.

The metabolite also disrupts intermediary metabolism contributing to metabolic acidosis.

The picture is thus one of a mixed alkalosis/acidosis phenomenon;

Question 40

How does salicylate overdose cause metabolic acidosis?

Answer 40

it causes uncoupling of oxidative phosphorylation and interruption of glucose and fatty acid metabolism

Question 41

Death in salicylate overdose is most commonly due to what?

Answer 41

cerebral and pulmonary edema (via increased capillary permeability) lead to ultimate demise if the patient is not decontaminated.

Question 42

Which NSAIDs should be avoided in elderly?

Answer 42

• Indomethacin (worst bleed risk)
• Ketorolac

all others should consider giving a PPI or misoprostol too

Question 43

T or F. Acetaminophen (tylenol) has no peripheral action

Answer 43

T. Not anti-inflammatory (not an NSAID)

Question 44

Acetaminophen (Tylenol) is most often associated with what AE?

Answer 44

acute hepatic failure

Question 45

Why not add a prostaglandin antagonist with chronic NSAID use?

Answer 45

not as effective (short duration of action)- PPIs are irreversible which is why they are so effective

Question 46

Which NSAID has the lowest CV risk?

Answer 46

Naproxen

Question 47

T or F. GCs can cause hyperlipidemia

Answer 47

T. As well as hyperglycemia