School of Health and Related Research (ScHARR), University of Sheffield, Sheffield, UK.
University Hospitals Birmingham NHS Foundation Trust, Birmingham, UK.
Health Technol Assess. 2017 Nov;21(68):1-170. doi: 10.3310/hta21680.
Non-infectious intermediate uveitis, posterior uveitis and panuveitis are a heterogeneous group of inflammatory eye disorders. Management includes local and systemic corticosteroids, immunosuppressants and biological drugs.
To evaluate the clinical effectiveness and cost-effectiveness of subcutaneous adalimumab (Humira; AbbVie Ltd, Maidenhead, UK) and a dexamethasone intravitreal implant (Ozurdex; Allergan Ltd, Marlow, UK) in adults with non-infectious intermediate uveitis, posterior uveitis or panuveitis.
Electronic databases and clinical trials registries including MEDLINE, EMBASE, Cochrane Database of Systematic Reviews, Database of Abstracts of Reviews of Effects and the World Health Organization's International Clinical Trials Registry Platform were searched to June 2016, with an update search carried out in October 2016.
Review methods followed published guidelines. A Markov model was developed to assess the cost-effectiveness of dexamethasone and adalimumab, each compared with current practice, from a NHS and Personal Social Services (PSS) perspective over a lifetime horizon, parameterised with published evidence. Costs and benefits were discounted at 3.5%. Substantial sensitivity analyses were undertaken.
Of the 134 full-text articles screened, three studies (four articles) were included in the clinical effectiveness review. Two randomised controlled trials (RCTs) [VISUAL I (active uveitis) and VISUAL II (inactive uveitis)] compared adalimumab with placebo, with limited standard care also provided in both arms. Time to treatment failure (reduced visual acuity, intraocular inflammation, new vascular lesions) was longer in the adalimumab group than in the placebo group, with a hazard ratio of 0.50 [95% confidence interval (CI) 0.36 to 0.70; < 0.001] in the VISUAL I trial and 0.57 (95% CI 0.39 to 0.84; = 0.004) in the VISUAL II trial. The adalimumab group showed a significantly greater improvement than the placebo group in the 25-item Visual Function Questionnaire (VFQ-25) composite score in the VISUAL I trial (mean difference 4.20; = 0.010) but not the VISUAL II trial (mean difference 2.12; = 0.16). Some systemic adverse effects occurred more frequently with adalimumab than with placebo. One RCT [HURON (active uveitis)] compared a single 0.7-mg dexamethasone implant against a sham procedure, with limited standard care also provided in both arms. Dexamethasone provided significant benefits over the sham procedure at 8 and 26 weeks in the percentage of patients with a vitreous haze score of zero ( < 0.014), the mean best corrected visual acuity improvement ( ≤ 0.002) and the percentage of patients with a ≥ 5-point improvement in VFQ-25 score ( < 0.05). Raised intraocular pressure and cataracts occurred more frequently with dexamethasone than with the sham procedure. The incremental cost-effectiveness ratio (ICER) for one dexamethasone implant in one eye for a combination of patients with unilateral and bilateral uveitis compared with limited current practice, as per the HURON trial, was estimated to be £19,509 per quality-adjusted life-year (QALY) gained. The ICER of adalimumab for patients with mainly bilateral uveitis compared with limited current practice, as per the VISUAL trials, was estimated to be £94,523 and £317,547 per QALY gained in active and inactive uveitis respectively. Sensitivity analyses suggested that the rate of blindness has the biggest impact on the model results. The interventions may be more cost-effective in populations in which there is a greater risk of blindness.
The clinical trials did not fully reflect clinical practice. Thirteen additional studies of clinically relevant comparator treatments were identified; however, network meta-analysis was not feasible. The model results are highly uncertain because of the limited evidence base.
Two RCTs of systemic adalimumab and one RCT of a unilateral, single dexamethasone implant showed significant benefits over placebo or a sham procedure. The ICERs for adalimumab were estimated to be above generally accepted thresholds for cost-effectiveness. The cost-effectiveness of dexamethasone was estimated to fall below standard thresholds. However, there is substantial uncertainty around the model assumptions. In future work, primary research should compare dexamethasone and adalimumab with current treatments over the long term and in important subgroups and consider how short-term improvements relate to long-term effects on vision.
This study is registered as PROSPERO CRD42016041799.
The National Institute for Health Research Health Technology Assessment programme.
非感染性中间葡萄膜炎、后葡萄膜炎和全葡萄膜炎是一组异质性的炎症性眼部疾病。治疗包括局部和全身皮质类固醇、免疫抑制剂和生物药物。
评估皮下阿达木单抗(Humira;AbbVie Ltd,英国梅登黑德)和地塞米松玻璃体内植入物(Ozurdex;Allergan Ltd,英国马洛)在非感染性中间葡萄膜炎、后葡萄膜炎或全葡萄膜炎成人患者中的临床疗效和成本效果。
电子数据库和临床试验注册库,包括 MEDLINE、EMBASE、Cochrane 系统评价数据库、疗效评价文摘数据库和世界卫生组织国际临床试验注册平台,检索至 2016 年 6 月,并于 2016 年 10 月进行了更新检索。
审查方法遵循已发布的指南。从国民保健制度和个人社会服务(PSS)的角度出发,开发了一个马尔可夫模型来评估地塞米松和阿达木单抗的成本效果,每种药物均与当前实践进行比较,时间范围为终生,参数采用已发表的证据。成本和效益以 3.5%贴现。进行了大量敏感性分析。
从筛选出的 134 篇全文文章中,有 3 项研究(4 篇文章)纳入了临床疗效评价。2 项随机对照试验(VISUAL I[活跃性葡萄膜炎]和 VISUAL II[非活跃性葡萄膜炎])比较了阿达木单抗与安慰剂,在这两个试验中,也提供了有限的标准治疗。与安慰剂组相比,阿达木单抗组的治疗失败时间(视力下降、眼内炎症、新血管病变)延长,风险比为 0.50[95%置信区间(CI)0.36 至 0.70;<0.001]在 VISUAL I 试验中,风险比为 0.57(95%CI 0.39 至 0.84;=0.004)在 VISUAL II 试验中。在 VISUAL I 试验中,阿达木单抗组在 25 项视觉功能问卷(VFQ-25)综合评分中比安慰剂组有显著改善(平均差异 4.20;=0.010),但在 VISUAL II 试验中差异无统计学意义(平均差异 2.12;=0.16)。阿达木单抗组比安慰剂组更频繁地出现一些全身不良反应。一项 RCT[HURON(活跃性葡萄膜炎)]比较了单次 0.7mg 地塞米松植入物与假手术,在这两个试验中,也提供了有限的标准治疗。与假手术相比,地塞米松在第 8 周和第 26 周时在玻璃体混浊评分零的患者百分比(<0.014)、平均最佳矫正视力改善(≤0.002)和 VFQ-25 评分至少提高 5 分的患者百分比(<0.05)方面有显著益处。地塞米松组比假手术组更频繁地出现眼内压升高和白内障。按照 HURON 试验,单侧单次地塞米松植入物在单侧和双侧葡萄膜炎患者中的组合与有限的当前治疗相比,其增量成本效果比估计为每获得一个质量调整生命年(QALY)19509 英镑。按照 VISUAL 试验,阿达木单抗用于主要双侧葡萄膜炎患者的增量成本效果比估计为每获得一个 QALY 在活跃性葡萄膜炎中为 94523 英镑,在非活跃性葡萄膜炎中为 317547 英镑。敏感性分析表明,失明率对模型结果的影响最大。在失明风险较高的人群中,这些干预措施可能更具成本效果。
临床试验并未完全反映临床实践。还确定了 13 项额外的具有临床相关性的对照治疗研究;然而,无法进行网络荟萃分析。由于证据基础有限,模型结果高度不确定。
2 项阿达木单抗的 RCT 和 1 项单侧单次地塞米松植入物的 RCT 显示与安慰剂或假手术相比有显著益处。阿达木单抗的 ICER 估计高于普遍接受的成本效果阈值。地塞米松的成本效果估计低于标准阈值。然而,模型假设存在很大的不确定性。在未来的研究中,应比较地塞米松和阿达木单抗与当前治疗方案在长期和重要亚组中的效果,并考虑短期改善与长期视力效果的关系。
本研究已在 PROSPERO CRD42016041799 注册。
英国国家卫生研究院卫生技术评估计划。
