|
|
Ed. Note: The following is a press
release from the American Heart Association.
March 4, 2007 -- Many doctors should change the
way they prescribe pain relievers for chronic pain in patients with or at
risk for heart disease based on accumulated evidence that nonsteroidal
anti-inflammatory drugs (NSAIDs), with the exception of aspirin, increase
risk for heart attack and stroke, according to an American Heart Association
statement published in Circulation: Journal of the American Heart
Association.
"We believe that some physicians have been prescribing the new COX-2
inhibitors as the first line of treatment. We are turning that around and
saying that, for chronic pain in patients with known heart disease or who
are at risk for heart disease, these drugs should be the last line of
treatment," said Elliott M. Antman, M.D., FAHA, lead author of the American
Heart Association scientific statement and Professor of Medicine at Harvard
Medical School and Brigham and Women's Hospital.
"We advise physicians to start with non-pharmacologic treatments such as
physical therapy and exercise, weight loss to reduce stress on joints, and
heat or cold therapy. If the non-pharmacologic approach does not provide
enough pain relief or control of symptoms, we recommend a stepped-care
approach when it comes to prescribing drugs," he added.
"Take into account the patient's health history and consider acetaminophen,
aspirin and even short-term use of narcotic analgesics as the first step. If
further relief is needed, physicians should suggest the least selective
COX-2 inhibitors first, moving progressively toward more selective COX-2
inhibitors, which are at the bottom of the list, only if needed. All drugs
should be used at the lowest dose necessary to control symptoms and
prescribed for the shortest time possible."
Drugs in the NSAIDs class work by inhibiting cyclooxygenase (COX), an enzyme
system that comes in two major forms: COX-1, which the body produces
constantly in most tissues, and COX-2, produced during the body's
inflammatory response. Because COX-1 is also protective of the
gastrointestinal (GI) tract, long-term use of drugs that suppress COX-1,
such as aspirin, have been associated with gastrointestinal complications,
including ulcers. "Selective" COX-2 inhibitors were developed to avoid the
GI complications of traditional NSAIDs, not because they had advantages in
terms of pain relief,
Antman explained. However, multiple studies have indicated an increased risk
of cardiovascular disease (CVD) complications from COX-2 selective NSAIDS,
particularly in patients with prior CVD or risk factors for CVD.
"Recent studies indicate that the cells lining the blood vessels have more
of the COX-2 enzyme than initially thought. So it's possible that inhibiting
the COX-2 pathway can make a person's blood more likely to clot. There is
also an increase in sodium and water retention, which in turn could worsen
heart failure and produce high blood pressure," Antman explained. "The more
you inhibit COX-1, the greater the increase in GI risk; the more you inhibit
COX-2 the greater the cardiovascular risk."
The scientific statement comes two years after the association released the
last one on the issue. It was prompted, in part, by new analyses indicating
that the increased cardiovascular risk associated with COX-2 selective
NSAIDs may also extend to less selective traditional NSAIDs.
The statement includes details from a meta-analysis indicating that,
compared with placebo, COX-2 selective drugs seem to increase the risk of a
heart attack by about 86 percent. The statement also points out that two
common NSAIDs traditionally thought of an non-selective -- diclofenac and
ibuprofen -- appear to increase the relative risk of cardiovascular disease.
In the last two years, the U.S. Food and Drug Administration (FDA) added
warning statements to NSAIDs, other than aspirin, pointing out the increased
risk for cardiovascular events.
One non-selective NSAID, naproxen, did not seem to increase CVD risk in
these analyses. However, Antman pointed out that although naproxen appeared
safer than the other NSAIDs, relatively few studies have been done with
naproxen and doctors should continue to be cautious about prescribing it as
well, pending more information.
"This is a fast-moving field with new information available from multiple
sources. We feel the most important thing the American Heart Association can
do is to give practical advice to clinicians who treat cardiac patients with
pain every day," said Antman.
Because there are so many drugs in the NSAID class and because they can
affect either COX-1 or COX-2 or both, it is very important to know where a
given drug falls in the range of selectivity, particularly when evaluating
the results of head-to-head comparisons of different drugs, Antman said. The
statement contains guidance that helps doctors see where individual drugs
lie on the continuum of COX-1 versus COX-2 selectivity.
Selective COX-2 inhibitors have been in the news since the FDA removed the
selective COX-2 inhibitor, rofecoxib, from the market in 2004. Since then,
other COX-2 selective drugs have been removed from the market in the United
States and other countries. One selective COX-2 inhibitor, celecoxib,
remains on the market, but warnings on it were strengthened and the FDA
advised that patients with a history of CVD or risk factors for CVD should
be informed of the possibility of increased risks from long-term use, Antman
said.
Co-authors include: Joel S. Bennett, M.D.; Alan Daugherty, Ph.D., D.Sc.,
FAHA; Curt Furberg, M.D., Ph.D., FAHA; Harold Roberts, M.D., FAHA and
Kathryn A. Taubert, Ph.D., FAHA.
Return To Table Of Contents |