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Musculoskeletal 2 > Pharm - OA > Flashcards

Pharm - OA Flashcards

1
Q

What is the place in therapy for topical NSAIDs in mild OA?

A

Considered over PO in patients with mild OA

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2
Q

What are the advantages of topical NSAIDs vs. PO NSAIDs?

A
  • useful for pain relief while avoiding serious system side effects
  • 60% receive 50% improvement in pain when compared to oral
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3
Q

What are the ADRs of topical NSAIDs?

A
  • prutitis
  • burning
  • pain
  • rash at application site
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4
Q

Name the topical NSAIDs

A
  • diclofenac (cream, gel, patch, solution)

- ketoprofen (cream, gel)

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5
Q

State the place in therapy for topical capsaicin

A

used when other products are ineffective or contraindicated

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6
Q

MOA for topical capsaicin

A

Alleviates pain through down-regulation of the TRPV1 receptor activity of nociceptive sensory neurons and maybe through depletion of substance P

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7
Q

Name the drugs that are topical capsaicins.

A
  • Capzasin

- Zostrix

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8
Q

ADRs of topical capsaicins

A

Burning, stinging, erythema at application site (usually gets better with repeat use)

**warn pt not to get it in their eyes/mouth and to wash hands after application

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9
Q

What is the appropriate dosing regimen for topical capsaicin?

A
  • must be used regularly, takes 2 weeks to take effect: gives preparation time to deplete substance P in nerve fibers supplying painful joints
  • application can be 2-4 times a day to affected joints (don’t have long term effects)
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10
Q

What is the place in therapy for PO NSAIDs in mod-severe OA?

A

consider on as-needed basis in patients who have insufficient relief with topical NSAIDs or have symptomatic OA in multiple joints (ex: spine and hip)

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11
Q

What GI toxicity is related to PO NSAID use?

A
  • minor: dyspepsia, anorexia, diarrhea (in 10-60%)

- major: GI bleeding and gastric mucosal injury - gastric/duodenal ulcers (in 7-13%)

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12
Q

What should you add to PO NSAID therapy to decrease GI toxicity?

A

**PPI

Use PPI with NSAIDs OR use celecoxib (COX-2) - can use Celecoxib and PPI in highest risk

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13
Q

What are the risk factors for GI toxicity in NSAID use?

A
  • increased age, hypertension, concomitant aspirin/corticosteroid use
  • H/o complicated ulcer, anticoagulant use, use of multiple NSAIDs over time
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14
Q

Cardiovascular toxicity related to PO NSAID use

A
  • CV thrombotic events
  • MI
  • Stroke
  • *risk increases with duration of use
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15
Q

Which patients are most appropriate to use COX-2 NSAID?

A
  • use with PPI for patients with increased GI risk (>70 y/o) without increased CV risk
  • if high risk to CV risk without as much GI risk: use naproxen + PPI
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16
Q

What are the risk factors for nephrotoxicity secondary to NSAID?

A
  • those with conditions associated with decreased renal blood flow: chronic renal insufficiency, CHF, severe hepatic disease, nephrotic syndrome)
  • those taking certain meds: diuretics, ACE inhibitors, cyclosporine, aminoglycosides
  • those of advanced age
17
Q

What are the clinical features of renal toxicity secondary to NSAID use?

A
  • increased serum creatinine and BUN
  • hyperkalemia
  • elevated BP
  • peripheral edema
  • weight gain
18
Q

Which patient allergy should cause you to avoid Celecoxib?

A

Contraindicated in patients with sulfa allergy

19
Q

What is the impact of nonselective NSAIDs on platelet function?

A

***ALL nonselective NSAIDs increase bleeding risk

  • aspirin inhibitors platelet aggregation irreversibly - bleeding time needs 5-7 days to normalize after stopping therapy
  • others inhibit platelet function reversibly with normalization 1-3 days after stopping
  • COX-2 selective NSAIDs have no bleeding risk but can increase CV events with increased thrombotic events
20
Q

What is the place in therapy for duloxetine in mod-severe OA?

A
  • for patients with OA in multiple joints and concomitant comorbidities that contraindicate NSAIDs
  • those who have not responded satisfactorily to NSAIDs
21
Q

What is the place in therapy for intra-articular glucocorticoids in mod-severe OA?

A

Can provide excellent pain relief, particularly when a joint effusion is present

22
Q

Which glucocorticoids are used for intra-articular injection?

A
  • Triamcinolone hexacetonide

- methylprednisolone acetate

23
Q

What are the systemic adverse effects secondary to intra-articular glucocorticoids?

A
  • hyperglycemia
  • edema
  • elevated BP
  • dyspepsia
  • rarely adrenal suppression

Blood glucose will rise within 24 hours to peak and then decline in next 3-5 days

Musculoskeletal 2 (14 decks)

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