Non-steroidal Anti-inflammatory Drugs For
Osteoarthritis: Villains Or Heroes?
Osteoarthritis (OA) is the most common form of
arthritis. It has been estimated that more than 20 million
Americans are afflicted with OA, and that number will rise to
40 million by the year 2020.
In recent months there has been a contentious debate between
cardiologists and rheumatologists regarding the use of
non-steroidal anti-inflammatory drugs (NSAIDS) for OA. Behind
this disagreement is controversy that exists as to the safest
and most effective way of treating OA, particularly with
respect to the use of NSAIDs, both non-selective and selective
(so-called COX-2 selective agents or coxibs). Adverse reactions
related to the gastrointestinal tract, particularly with the
non-selective NSAIDs, have been described. And, more recently,
concerns have been raised regarding cardiovascular events with
both groups of agents.
A recent scientific statement from the American Heart
Association (AHA) made recommendations with regard to the
treatment of OA. (E.M. Antman, J.S. Bennett, A. Daugherty, C.
Furberg, H. Roberts, K.A. Taubert, Use of nonsteroidal
antiinflammatory drugs. An update for clinicians: a scientific
statement from the American Heart Association, Circulation.
2007;113:2906-2913). The recommendations come in the form of
guidelines. These include:
COX-2 inhibition can result in an increased risk for thrombosis
due to increased activity of thromboxane A2 and reduced
activity of prostacyclin. In addition, all NSAIDs can increase
sodium and water retention, increasing the risk for
exacerbations of hypertension and heart failure. Finally, COX-2
up-regulation may reduce myocardial ischemia and infarction
during acute cardiac events, and inhibition of this isoenzyme
can increase infarct size and lead to myocardial rupture.
"Nonselective" NSAIDs also differ with regard to COX
selectivity. Diclofenac has greater COX-2 selectivity than
ibuprofen, which in turn has greater COX-2 selectivity compared
with naproxen.
Initial treatment of musculoskeletal pain should include
nonpharmacologic therapy, including physical therapy,
heat/cold, and orthotics. Acetaminophen and aspirin are
probably the best initial choices for analgesia, although these
agents should be used at the lowest possible dose for the
shortest possible period.
For patients who fail conservative therapy for musculoskeletal
pain, NSAIDs may be chosen as a next step. Clinicians and
patients should realize that the use of NSAIDs may slightly
increase the risk for cardiovascular and cerebrovascular
events. With this in mind, clinicians should try to use NSAIDs
with lower selectivity for COX-2.
Naproxen is probably the NSAID associated with the lowest risk
for thrombosis. The Alzheimer's Disease Anti-inflammatory
Prevention Trial (ADAPT) questioned the safety of naproxen, but
this trial had significant limitations.
Patients with a history of gastrointestinal tract bleeding or
who are at high risk for bleeding who require analgesia should
be prescribed acetaminophen first. For these patients who
require NSAID therapy, proton-pump inhibitors have been
demonstrated to reduce the risk for recurrent gastrointestinal
tract bleeding among patients receiving low-dose aspirin.
Patients with active atherosclerotic processes are at increased
risk for the thromboembolic complications of COX-2 inhibitors.
Renal function and blood pressure should be monitored during
treatment with COX-2 inhibitors.
Ibuprofen, but not acetaminophen or diclofenac, appears to
reduce the physiologic efficacy of aspirin in preventing
thrombosis. Current recommendations call for delaying ibuprofen
dosing until at least 30 minutes after taking aspirin or at
least 8 hours prior to aspirin dosing.
The upshot? Use NSAIDS for OA as a last resort!
In an editorial in the journal, Osteoarthritis and Cartilage, a
panel of arthritis research experts has vehemently- and not
surprisingly- disagreed with these proposals.
The editorial summarizes the outcomes of an international
workshop organized by the Osteoarthritis Research Society
International (OARSI) and the International COX-2 Study Group,
held 24--25 March 2007. (R.W. Moskowitz, S. Abramson, F
Berenbaum, L.S.Simon, M. Hochberg, Coxibs and NSAIDS - Is the
air any clearer? Perspectives from the OARSI international
COX-2 workshop 2007, Osteoarthritis and Cartilage.
2007;15:849-856).
The authors urge that an evidence-based approach must be taken
when making recommendations to patients.
The editorial questions the recommendation made in the AHA
statement which described a stepped care approach to
pharmacologic therapy for musculoskeletal diseases.
The authors also strongly recommend that several aspects of the
AHA statement be reconsidered. For example, they urge that the
AHA withdraw their non-evidence-based recommendations that
high-dose aspirin be administered alone as a first line therapy
for patients with chronic pain and arthritis.
Dr Roland W. Moskowitz, Professor of Medicine at Case Western
Reserve University/University Hospitals of Cleveland and the
lead author of the editorial commented, "Careful review of the
pros and cons of using these agents, and the situations in
which they are most safely and effectively used, is required to
help us understand how best to take advantage of their
availability".
The upshot of this
whole discussion is that rheumatologists and cardiologists
differ in their approach. It becomes an issue of gut feeling
versus evidence. What needs to be considered is not only data
regarding cardiovascular risk which is still far from clear but
also the effects on the quality of life for patients with OA.
Stay tuned!
By: Nathan Wei
Article
Directory:
http://www.articledashboard.com
Nathan Wei, MD FACP
FACR is a rheumatologist and Director of the Arthritis and
Osteoporosis Center of Maryland. He is a Clinical Assistant
Professor of Medicine at the University of Maryland School of
Medicine. For more info: Arthritis
Treatment
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