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A five-year model to assess the early cost-effectiveness of new diagnostic tests in the early diagnosis of rheumatoid arthritis

机译:五年模型评估类风湿关节炎的早期诊断中新诊断测试的早期成本效益

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Background There is a lack of information about the sensitivity, specificity and costs new diagnostic tests should have to improve early diagnosis of rheumatoid arthritis (RA). Our objective was to explore the early cost-effectiveness of various new diagnostic test strategies in the workup of patients with inflammatory arthritis (IA) at risk of having RA. Methods A decision tree followed by a patient-level state transition model, using data from published literature, cohorts and trials, was used to evaluate diagnostic test strategies. Alternative tests were assessed as add-on to or replacement of the ACR/EULAR 2010 RA classification criteria for all patients and for intermediate-risk patients. Tests included B-cell gene expression (sensitivity 0.60, specificity 0.90, costs €150), MRI (sensitivity 0.90, specificity 0.60, costs €756), IL-6 serum level (sensitivity 0.70, specificity 0.53, costs €50) and genetic assay (sensitivity 0.40, specificity 0.85, costs €750). Patients with IA at risk of RA were followed for 5?years using a societal perspective. Guideline treatment was assumed using tight controlled treatment based on DAS28; if patients had a DAS28 >3.2 at 12?months or later patients could be eligible for starting biological drugs. The outcome was expressed in incremental cost-effectiveness ratios (€2014 per quality-adjusted life year (QALY) gained) and headroom. Results The B-cell test was the least expensive strategy when used as an add-on and as replacement in intermediate-risk patients, making it the dominant strategy, as it has better health outcomes and lower costs. As add-on for all patients, the B-cell test was also the most cost-effective test strategy. When using a willingness-to-pay threshold of €20,000 per QALY gained, the IL-6 and MRI strategies were not cost-effective, except as replacement. A genetic assay was not cost-effective in any strategy. Probabilistic sensitivity analysis revealed that the B-cell test was consistently superior in all strategies. When performing univariate sensitivity analysis for intermediate-risk patients, specificity and DAS28 in the B-cell add-on strategy, and DAS28 and sensitivity in the MRI add-on strategy had the largest impact on the cost-effectiveness. Conclusions This early cost-effectiveness analysis indicated that new tests to diagnose RA are most likely to be cost-effective when the tests are used as an add-on in intermediate-risk patients, and have high specificity, and the test costs should not be higher than €200–€300. Electronic supplementary material The online version of this article (doi:10.1186/s13075-016-1020-3) contains supplementary material, which is available to authorized users.
机译:背景缺乏关于敏感性,特异性和成本的信息,新的诊断测试应改善风湿性关节炎(RA)的早期诊断。我们的目标是探讨各种新诊断测试策略在具有RA风险的炎性关节炎(IA)患者的检查中的早期成本效益。方法使用决策树和患者水平的状态转换模型,并使用来自公开文献,队列和试验的数据评估诊断测试策略。评估所有患者和中危患者的替代测试作为ACR / EULAR 2010 RA分类标准的补充或替代。测试包括B细胞基因表达(敏感性0.60,特异性0.90,费用€150),MRI(敏感性0.90,特异性0.60,费用€756),IL-6血清水平(敏感性0.70,特异性0.53,费用€50)和遗传分析(灵敏度0.40,特异性0.85,费用750欧元)。从社会角度对IA有RA风险的患者随访5年。假设采用基于DAS28的严格对照治疗进行指导治疗;如果患者在12个月或更晚时DAS28> 3.2,则有资格开始使用生物药物。结果以增加的成本效益比(每个质量调整生命年(QALY)获得2014欧元)和净空来表示。结果B细胞测试在中度风险患者中用作附加疗法和替代疗法时,是最便宜的策略,使其成为主要策略,因为它具有更好的健康效果和更低的成本。作为所有患者的附加工具,B细胞测试也是最经济高效的测试策略。当使用每获得QALY 20,000欧元的支付意愿阈值时,IL-6和MRI策略不是有效的方法,除非可以替代。遗传测定在任何策略中都不具有成本效益。概率敏感性分析表明,在所有策略中,B细胞测试始终具有优越性。在对中危患者进行单变量敏感性分析时,B细胞添加策略中的特异性和DAS28以及MRI附加策略中的DAS28和敏感性对成本效益的影响最大。结论这项早期的成本效益分析表明,将诊断为RA的新检测方法用作中度风险患者的附加检测方法最有可能具有成本效益,并且具有较高的特异性,因此不应将检测费用高于€200-€300。电子补充材料本文的在线版本(doi:10.1186 / s13075-016-1020-3)包含补充材料,授权用户可以使用。

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