Meta-analysis of treatment termination rates among rheumatoid arthritis patients receiving disease-modifying anti-rheumatic drugs

doi:10.1093/rheumatology/39.9.975

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Rheumatology 2000; 39: 975-981
© 2000 British Society for Rheumatology

Meta-analysis of treatment termination rates among rheumatoid arthritis patients receiving disease-modifying anti-rheumatic drugs

A. Maetzel, A. Wong, V. Strand¹, P. Tugwell², G. Wells and C. Bombardier³

University Health Network, Toronto, Ontario, Canada
¹ Division of Immunology, Stanford University, Stanford CA, USA,
² Department of Medicine and The Loeb Health Research Institute, Clinical Epidemiology Unit, University of Ottawa, Ontario,
³ Arthritis & Autoimmunity Research Centre, University Health Network, Toronto, Ontario and Clinical Epidemiology and Healthcare Research Program, University of Toronto, Ontario, Canada

Objective. To summarize the evidence on treatment withdrawalrates reported in observational studies and randomized controlledtrials (RCTs) of methotrexate (MTX), parenteral gold (GST),sulphasalazine (SSZ) and hydroxychloroquine (HCQ) among patientswith rheumatoid arthritis (RA).

Methods. Two independent Medline searches were used toretrieve relevant studies published between 1966 and 1997. Thosewhich disclosed information on the number of patients withdrawingfrom the drug were retained. Cumulative probabilities of survivalon treatment were then computed using actuarial survival estimates,and differences were tested using log-rank, Wilcoxon and Coxproportional hazards tests.

Results. A total of 159 studies provided withdrawal information,and the numbers of patients who withdrew, in general or becauseof inefficacy or toxicity, could be abstracted from 110 studiescontributing 142 treatment arms (MTX, 48; GST, 56; SSZ, 22;HCQ, 16). Data for HCQ were available only up to 24 months,but combined percentages of patients estimated to have continuedMTX, GST or SSZ, respectively, for 60 months were 36, 23 and22% when all failures were considered, 75, 73 and 53% when withdrawalsdue to lack of efficacy alone were considered, and 65, 36 and48% when only withdrawals due to toxicity were taken into account.The Cox proportional hazards test performed on all withdrawals,after adjusting for year of publication and type of study, revealedthat patients remained on MTX significantly longer than theydid on the other three agents; however, the patients stayedsignificantly longer on GST than MTX when withdrawals for inefficacywere analysed separately. No significant differences in withdrawalrates were noted between observational studies and RCTs.

Conclusion. Patients with RA stay significantly longeron MTX than on other disease-modifying anti-rheumatic drugs.Higher withdrawal rates among those given GST are mainly dueto high toxicity, whereas the majority of withdrawals from SSZand HCQ result from lack of efficacy. Withdrawal rates in observationalstudies are similar to those reported in RCTs.

Correspondence to: A. Maetzel, University Health Network, 610University Avenue, Room 16-741, Toronto, Ontario M5G 2M9, Canada.

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