ORIGINAL ARTICLE
Modeling and cost-effectiveness analysis of etanercept in adults with rheumatoid arthritis in Japan: a preliminary analysis
Authors
Makoto Tanno1 , Ichiro Nakamura1, Katsumi Ito1, Hidekazu Tanaka2, Hisahiko Ohta3, Makoto Kobayashi4, Akitoshi Tachihara5, Masakazu Nagashima5, Shinichi Yoshino5 and Atsuo Nakajima5
| (1) |
Department of Rheumatology, Yugawara Kosei-Nenkin Hospital, 438 Miyakami, Yugawara-cho, Ashigarashimo-gun, Kanagawa 259-0314, Japan |
| (2) |
Department of Rheumatology, Tokyo Metropolitan Rehabilitation Hospital, Sumida-ku, Tokyo, Japan |
| (3) |
Department of Health Service Administration, Nippon Medical School, Bunkyo-ku, Tokyo, Japan |
| (4) |
Crecon Research and Consulting Inc., Shibuya-ku, Tokyo, Japan |
| (5) |
Department of Joint Disease and Rheumatism, Nippon Medical School, Bunkyo-ku, Tokyo, Japan |
Received:
18 November 2005
Accepted:
08 February 2006
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Abstract
The tumor necrosis factor (TNF) antagonist etanercept is an antirheumatic agent which was approved by Japanese regulatory authorities in January 2005. In Japan, the cost-effectiveness of this therapy for patients with rheumatoid arthritis (RA) has not previously been evaluated. This study models the cost-utility of etanercept in comparison with standard therapy with disease-modifying antirheumatic drugs (DMARDs) among adult Japanese RA patients who have failed a previous course of the DMARD bucillamine. A Markov model with 6-month cycles was constructed to compare two therapeutic strategies: etanercept versus standard therapy. For each cycle, one of three options was possible: a patient could (i) remain on current therapy if American College of Rheumatology criteria for 20% clinical improvement (ACR20) were achieved, (ii) switch to another drug in the therapeutic pathway if ACR20 was not achieved or if side effects severe enough to cause treatment discontinuation occurred, or (iii) they could die. The therapeutic pathway for the etanercept strategy was etanercept, methotrexate (MTX), sulfasalazine (SSZ), combination therapy (MTX + SSZ) and, finally, no DMARD. The pathway for standard therapy was identical except the initial therapy was MTX (etanercept was excluded). Results from clinical trials in U.S. and European patient populations were used to derive model probabilities for disease progression, response to drug therapy, and relationships between ACR20 response and functional improvement as measured by the Health Assessment Questionnaire (HAQ) disability index. An equation was developed to predict utility from HAQ scores of Japanese patients. Costs for drugs and medical services in Japan were obtained for April 2003. Analysis was conducted from a societal perspective, including lost productivity costs due to RA disability and premature mortality. Costs were discounted at 6% annually, and quality-adjusted life years (QALYs) at 1.5% annually. Model parameters were varied by 20% above and below base-case values in sensitivity analyses. Compared to standard therapy, the etanercept strategy was \6.39 million more costly per patient but yielded an additional 2.56 QALYs. The incremental cost-utility ratio was \2.50 million/QALY. Sensitivity analyses revealed that cost-utility was most strongly influenced by the acquisition cost of etanercept and the percentage of etanercept recipients who achieved ACR20. Using commonly applied thresholds for acceptable cost-effectiveness in the United States ($50000 = \5.5 million/QALY) and the United Kingdom (£30000 = \5.7 million/QALY), etanercept therapy in Japan can be considered cost-effective. Cost-utility ratios did not exceed these thresholds in any sensitivity analysis. Further analyses should be conducted once clinical and epidemiologic data for Japanese patients become available.
Key words
Anti-tumor necrosis factor (TNF)-α - Cost-effectiveness analysis - Disease-modifying antirheumatic drug (DMARD) - Etanercept - Japan - Rheumatoid arthritis (RA) |
