The Therapeutic Goods Administration (TGA) of Australia has introduced new measures on the prescribing of anti-arthritis
drugs known as Cox-2 inhibitors following the findings of a review into the safety of this family of medicines.
In September last year the popular arthritis drug, Vioxx, was withdrawn from the market world wide because medical trials had
shown a significant increased risk of heart attacks and strokes.
In response, the TGA undertook urgent evaluations of new information provided by the sponsoring pharmaceutical companies of
all other registered Cox-2 inhibitor drugs.
The results of this review were considered by the Australian Drug Evaluation Committee (ADEC) which made a number of
recommendations to restrict the use of these drugs in Australia.
As a result, the TGA will immediately require manufacturers of Cox-2 inhibitors to place new highlighted explicit warnings in
product information about the increased risk of cardiovascular adverse events from this group of drugs. The new warning
statements are to be highlighted with a black boxed margin.
The TGA is also advising people who are taking more than 200mg a day of celecoxib (Celebrex) or more than 15 mg a day of
meloxicam (Mobic; Movalis) to review their treatment regime with their doctors.
The TGA believes that most Australians using these drugs will be taking low doses that already meet this dosage advice, but
some patients, particularly with rheumatoid arthritis or a rare bowel condition, may be taking 400 mg or 800 mg of celecoxib
a day and some patients with arthritis may be taking more than 15 mg of meloxicam a day.
This recommended dose reduction may result in some patients with arthritis having increased symptoms but the review of Cox-2
inhibitors clearly indicated there is an increased risk of heart attacks and strokes with high doses of these drugs.
ADEC reviewed evidence of six drugs in the Cox-2 inhibitor family, all of which were considered to be have risks associated
with their use.
It determined that the exact size of the risk and the exact duration of therapy associated with increased risk are still
unknown, and so have recommended that Cox-2 inhibitors should be prescribed only when other treatments cannot be tolerated or
have caused serious adverse effects.
In addition celecoxib and meloxicam should not be prescribed for patients with increased risks of cardiovascular events, such
as heart attacks, and treatment should be limited to the shortest time needed.
Concerning celecoxib, the Committee took into account the results of a study of celecoxib 800 mg a day in low cardiovascular
risk patients which showed an increased risk of cardiovascular event. The results of studies of 400 mg a day of celecoxib in
low cardiovascular risk patients are conflicting with one study at this dose level finding an increased risk.
On the other hand, several recently published papers describing observational studies of patients using large linked medical
record databases in North America have not reported an increased myocardial infarction risk with celecoxib. Dose analysis was
not undertaken in all studies but it is likely that a large majority of patients were taking 200 mg/day or less. Such
observations are consistent with the preliminary results of an Australian case-control study, the results of which were made
available to ADEC. An increased risk of acute coronary syndrome was not found for the patients that were studied. Very few of
these Australian patients were taking more than 200 mg a day of celecoxib.
Concerning meloxicam, there are theoretical grounds for regarding the drug as having reduced cardiovascular risks. The drug
has less selective Cox-2 inhibition than celecoxib or rofecoxib. Clinical study data are more meagre, with most studies
limited to no more than six months duration. The Committee notes that a Prescription Event Monitoring study in the UK and an
observational study in Quebec, Canada, provided reassurance that the cardiovascular risk at up to 15 mg is acceptable. ADEC
recommended that further research be conducted.
The new requirements reinforce and extend advice given to Australian heath care professionals in the Australian Adverse Drug
Reactions Bulletin, October 2003, and repeated in December 2004.
The TGA has also accepted a number of other recommendations of ADEC and has given notice to the relevant companies:
-- it is proposed to cancel the registration of the drug parecoxib (Dynastat) because of the risk of cardiovascular events.
Dynastat is marketed in Australia and is approved as a single dose at the time of surgery to reduce post-operative pain;
-- it is proposed to withdraw the indication of management of arthritis of the drug valdecoxib (Valdyne, Dynoral - known in
some countries as Bextra) which is converted to parecoxib in the body. Valdecoxib has not been marketed in Australia.
Valdecoxib has been associated with an increased risk of cardiovascular events in cardiac by-pass graft patients. The use of
Valdecoxib for 5 days as an analgesic in patients without increased cardiovascular risk will remain;
-- it is proposed to greatly limit the approved uses of two other Cox-2 inhibitors which have not yet been marketed in
Australia. They are etoricoxib and lumiracoxib. In both instances, ADEC was not sufficiently assured of the safety of these
drugs for anything other than short term use in patients without increased cardiovascular risk.
Concerning parecoxib and valdecoxib, ADEC noted reports of two published studies in which valdecoxib alone for 14 days and
parecoxib followed by valdecoxib for 10 days were associated with increased risk of cardiovascular events in patients
undergoing coronary artery bypass graft surgery. The Committee was not assured from other available data that the safety of
parecoxib in other surgical patients or the safety of valdecoxib other than when used for short periods in patients without
cardiovascular risk, had been studies adequately.
Printable version of Expanded
information on Cox-2 inhibitors for doctors and pharmacists media statement
People who are concerned about their use of Cox-2 inhibitors should discuss their treatment with their medical practitioner.
Dr John McEwen
Principal Medical Adviser
10th February 2005
This is a press release from the Australian Dept
of Health
View drug information on Bextra; Vioxx.
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