Comparison of the incidence rates of thromboembolic events reported for patients prescribed rofecoxib and meloxicam in general practice in England using prescription-event monitoring (PEM) data

doi:10.1093/rheumatology/keg379

Rheumatology Advance Access originally published online on June 27, 2003

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Rheumatology 2003; 42: 1342-1353
© 2003 British Society for Rheumatology

Comparison of the incidence rates of thromboembolic events reported for patients prescribed rofecoxib and meloxicam in general practice in England using prescription-event monitoring (PEM) data

D. Layton¹^,2, E. Heeley¹, K. Hughes¹ and S. A. W. Shakir¹^,2

¹Drug Safety Research Unit, Bursledon Hall, Blundell Lane, Southampton and ²University of Portsmouth, UK.

Correspondence to: D. Layton. E-mail: deborah.layton{at}dsru.org

Background. Rofecoxib and meloxicam are classified as cyclo-oxygenase(COX)-2 selective inhibitors. The Drug Safety Research Unit(DSRU) monitored the post-marketing safety of these drugs inEngland using the non-interventional observational cohort techniqueof prescription-event monitoring (PEM).

Objectives. To compare the incidence rates of selected thromboembolic(TE)(cardiovascular, cerebrovascular and peripheral venous thrombotic)events reported for patients prescribed rofecoxib and meloxicamin general practice.

Methods. Patients were identified from dispensed prescriptionswritten by general practitioners (GPs) for meloxicam (December1996 to March 1997) and rofecoxib (July to November 1999). Simplequestionnaires requesting details of events recorded during/aftertreatment, indication and potential risk factors (includingage, sex and NSAIDs prescribed within 3 months of treatment)were posted to prescribing GPs approximately 9 months afterthe first prescription for each patient. Incidence rates ofthe first event within each TE group were calculated; crudeand age- and sex-adjusted rate ratios (RR) obtained using regressionmodelling.

Results. During the 9 months after starting treatment, 21 (0.14%)and 19 (0.10%) patients were reported to have cardiovascularTE events, and 74 (0.48%) and 52 (0.27%) cerebrovascular TEevents, and 6 (0.05%) and 20 (0.10%) were reported to have peripheralvenous thrombotic events for rofecoxib and meloxicam, respectively.Regarding time to first event, there was a persistent divergencebetween the two drugs from the start of treatment for both thecerebrovascular TE event group (log rank test P = 0.0063) andthe peripheral venous thrombotic event group (log rank testP = 0.0264). Indication and use of a NSAID within 3 months priorto starting treatment had no statistically significant effecton the relative risk estimates of the event groups and was excludedfrom subsequent analyses. Adjusting for the two identified riskfactors of age (age²) and sex, for rofecoxib the adjusted cerebrovascularTE event group rate was higher than for meloxicam [RR 1.68 (95%CI 1.15, 2.46)]; lower than meloxicam for the peripheral venousthrombotic event group [RR 0.29 (95% CI 0.11, 0.78)], and notdifferent for the cardiovascular TE event group [RR 1.38 (95%CI 0.71, 2.67)].

Conclusions. This study reports a relative increase in the rateof cerebrovascular TE events and a relative reduction in peripheralvenous thrombotic events in users of rofecoxib compared withmeloxicam. There was no difference in the rate of cardiovascularthromboembolic events. The incidence of these three groups ofevents reported in each of these two drug cohorts was low (lessthan 0.5%), therefore the relevance of our findings needs tobe taken into consideration with other clinical and pharmacoepidemiologicalstudies.

KEY WORDS: COX-2 selective inhibitors, Rofecoxib, Meloxicam, Adverse events, Prescription-event monitoring, Drug safety.

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