1 Wake Forest University School of Medicine, Winston-Salem, North Carolina.
2 U.S. Health Economics & Outcomes Research.
J Manag Care Spec Pharm. 2017 May;23(5):583-589. doi: 10.18553/jmcp.2017.23.5.583.
Patients with moderate-to-severe psoriasis may be treated with above-label doses of biologics in an attempt to optimize outcomes. Dose escalation will have an effect on the cost of treatment.
To examine costs related to above-label use of etanercept, adalimumab, and ustekinumab among patients with moderate-to-severe psoriasis.
A retrospective study was performed using a large U.S. claims database. Patients were included in the study if they were aged ≥ 18 years with a diagnosis of psoriasis (excluding psoriatic arthritis) and had at least 1 medication fill for etanercept, adalimumab, or ustekinumab between January 1, 2011, and June 30, 2012. In addition, patients were required to have continuous enrollment for 12 months before, and 18 months after, the first biologic use (index biologic) during the maintenance period (defined as the period following the induction period in which each agent was titrated to its recommended maintenance dose per label) and at least 1 prescription filled for the index biologic during the 18 months after the maintenance period. Extensive above-label use was defined as taking an above-label dose (at least 10% higher than indicated in the label) for ≥ 180 days over a 12-month period following the maintenance period. Percentages of patients with extensive above-label use, mean number of days of above-label use, and additional costs associated with extensive above-label use (abovelabel cost minus on-label cost) were examined.
The study included 3,310 patients who started treatment with etanercept (n = 1,443), adalimumab (n = 1,447), or ustekinumab (n = 420). Extensive above-label use occurred in 20.0% of etanercept patients, 2.6% of adalimumab patients, and 14.8% of ustekinumab patients. The mean duration of extensive above-label use was roughly similar for the 3 biologics (mean days [±SD]: 282 [±55] for etanercept, 279 [±57] for adalimumab, and 305 [±43] for ustekinumab). Additional annual costs per patient because of extensive above-label use were $19,458 for etanercept, $18,972 for adalimumab, and $21,045 for ustekinumab. Total additional annual costs were $5,623,362 for etanercept, $701,964 for adalimumab, and $1,304,790 for ustekinumab.
Psoriasis patients treated with etanercept, adalimumab, or ustekinumab had extensive above-label use over the 12-month follow-up period, which subsequently led to higher costs.
Novartis Pharmaceuticals Corporation sponsored this study and the resultant publication. BioScience Communications provided medical writing and editorial support, which was also funded by Novartis Pharmaceuticals Corporation. Feldman was engaged by Novartis Pharmaceuticals as a paid clinical expert and scientific advisor for this study. He has received research support and speaking and/or consulting fees from AbbVie, Advance Medical, Amgen, Anacor, Astellas, Baxter, Boehringer Ingelheim, Caremark, Celgene, Eli Lilly, Galderma, GSK/Stiefel, Informa, Janssen, LEO Pharma, Merck, Merz, Mylan, National Biological, National Psoriasis Foundation, Pfizer, Qurient, Suncare Research, UpToDate, and Valeant; is the founder and majority owner of www.DrScore.com ; and is founder and part owner of Causa Research. Zhao, Herrera, Tian, and Li are employees of Novartis Pharmaceuticals. Zhou is a paid consultant for Novartis Pharmaceuticals and is an employee of KMK Consulting. Study concept and design were contributed by Feldman, Zhao, Herrera, and Li. Zhou and Li were responsible for data collection. Data were interpreted by Feldman and Zhao, with assistance from Zhou, Herrera, Tian, and Li. The manuscript was written primarily by Feldman and Zhao, with assistance from Zhou and Li. The manuscript was revised by Feldman and Zhao, assisted by Zhou, Herrera, Tian, and Li. Portions of this work were presented at the 34th Anniversary Fall Clinical Dermatology Conference in Las Vegas, Nevada, October 1-4, 2015.
中重度银屑病患者可能会使用标签外剂量的生物制剂进行治疗,以优化治疗效果。剂量升级会影响治疗成本。
研究中重度银屑病患者使用依那西普、阿达木单抗和乌司奴单抗的标签外使用相关成本。
采用美国大型索赔数据库进行回顾性研究。入选标准为:年龄≥18 岁,诊断为银屑病(不包括银屑病关节炎),且在 2011 年 1 月 1 日至 2012 年 6 月 30 日期间至少有 1 次依那西普、阿达木单抗或乌司奴单抗的用药记录。此外,患者在维持期(诱导期后每个药物都根据标签推荐维持剂量滴定的时期)开始使用生物制剂前 12 个月和使用生物制剂后 18 个月内必须持续参保,并且在维持期后 18 个月内至少有 1 次处方记录用于索引生物制剂。广泛标签外使用定义为在维持期后 12 个月内,每日使用标签外剂量(至少比标签上的指示剂量高 10%)超过 180 天。研究考察了广泛标签外使用患者的比例、平均标签外使用天数以及与广泛标签外使用相关的额外成本(标签外成本减去标签内成本)。
本研究共纳入 3310 名开始接受依那西普(n=1443)、阿达木单抗(n=1447)或乌司奴单抗(n=420)治疗的患者。依那西普、阿达木单抗和乌司奴单抗患者中广泛标签外使用的比例分别为 20.0%、2.6%和 14.8%。3 种生物制剂的平均标签外使用持续时间大致相似(依那西普患者:平均 282 [±55] 天,阿达木单抗患者:平均 279 [±57] 天,乌司奴单抗患者:平均 305 [±43] 天)。由于广泛标签外使用,每位患者每年额外成本分别为依那西普 19458 美元、阿达木单抗 18972 美元和乌司奴单抗 21045 美元。依那西普、阿达木单抗和乌司奴单抗每年的总额外成本分别为 5623362 美元、701964 美元和 1304790 美元。
接受依那西普、阿达木单抗或乌司奴单抗治疗的银屑病患者在 12 个月的随访期间有广泛的标签外使用,这导致了更高的成本。
诺华制药公司赞助了这项研究和相关出版物。BioScience Communications 提供了医学写作和编辑支持,该支持也由诺华制药公司资助。Feldman 受雇于诺华制药公司,担任该研究的付费临床专家和科学顾问。他曾因 AbbVie、Advance Medical、Amgen、Anacor、Astellas、Baxter、Boehringer Ingelheim、Caremark、Celgene、Eli Lilly、Galderma、GSK/Stiefel、Informa、Janssen、LEO Pharma、Merck、Merz、Mylan、National Biological、National Psoriasis Foundation、Pfizer、Qurient、Suncare Research、UpToDate 和 Valeant 接受过研究资助和演讲和/或咨询费;他是 www.DrScore.com 的创始人兼多数股权所有者;他还是 Causa Research 的创始人兼部分所有者。Zhao、Herrera、Tian 和 Li 是诺华制药公司的员工。Zhou 是诺华制药公司的付费顾问,也是 KMK Consulting 的员工。研究的概念和设计由 Feldman、Zhao、Herrera 和 Li 贡献。Zhou 负责数据收集。Feldman 和 Zhao 对数据进行了解释,并得到了 Zhou、Herrera、Tian 和 Li 的协助。主要由 Feldman 和 Zhao 撰写手稿,得到了 Zhou 和 Li 的协助。Zhou、Herrera、Tian 和 Li 对草稿进行了修订。工作的一部分在 2015 年 10 月 1 日至 4 日在拉斯维加斯举行的第 34 届年度秋季临床皮肤科会议上进行了介绍。
