克罗恩病患者起始生物制剂治疗模式和维持剂量滴定的3年随访评价

IF 2.3 Q2 ECONOMICS Journal of Health Economics and Outcomes Research Pub Date : 2023-11-20 eCollection Date: 2023-01-01 DOI:10.36469/001c.88947
Ruizhi Zhao, Zhijie Ding, Parul Gupta, Laurence Gozalo, Robert Bruette, Victor M Johnson, Keshia Maughn, Yihang Liu, Sumesh Kachroo
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引用次数: 0

摘要

背景:克罗恩病(CD)患者启动生物制剂治疗模式的实际证据有限,随访时间较长。这项研究描述了3年随访的乳糜泻患者的持续性和剂量滴定。方法:本回顾性观察研究采用STATinMED RWD Insights全付费医疗和药学数据进行。确定了2016年9月至2018年10月期间至少有1项CD医疗索赔和至少1项生物制剂(阿达木单抗[ADA], certolizumab pegol (CZP),英夫利昔单抗[IFX]及其生物仿制药产品[IFX- bs], ustekinumab [UST]和vedolizumab [VDZ])的医疗/药房索赔的成年患者。商业保险患者在生物制剂开始治疗前至少12个月和开始治疗后至少36个月被选中。确诊的乳糜泻患者被纳入最后的队列。评估基线患者特征和3年随访期间的治疗模式。结果汇总采用均值和标准差或计数和百分比。结果:共发现2309例确诊CD患者(IFX 847例[36.7%],ADA 534例[23.1%],VDZ 486例[21.1%],UST 394例[17.1%],CZP 85例[3.7%],IFX- bs 72例[3.1%])。由于样本量小,排除了CZP和IFX-BS。大约一半的乳糜泻患者年龄在35到54岁之间。UST患者的Charlson合并症指数评分较高。常见的合并症(>10%)包括贫血、焦虑、抑郁和高血压。在3年随访中,UST患者的持续时间最长(61.4%),其次是VDZ (58.0%), ADA(52.1%)和IFX(48.1%)。ADA的停药率最高(37.3%),其次是UST(30.7%)、IFX(28.1%)和VDZ(25.3%)。在3年随访中,IFX的剂量滴定率最高(76.5%),UST的剂量滴定率最低(50.8%)。特别是,UST具有最低的剂量递增率(35.5%)和最高的剂量减少率(16.5%)。结论:在3年的随访期间,不同生物制剂使用者中CD患者的持续时间最长,剂量递增最低,可能表明UST具有更好的临床反应。为了更好地了解生物制剂使用者的治疗模式,未来的研究需要对混杂因素进行更长的随访调整。
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Evaluation of Treatment Patterns and Maintenance Dose Titration Among Patients With Crohn's Disease Initiating Biologics With 3 Years of Follow-Up.

Background: There is limited real-world evidence on treatment patterns of patients with Crohn's disease (CD) initiating biologics with an extensive follow-up period. This study describes persistence and dose titration among CD patients with 3 years of follow-up. Methods: This retrospective observational study was conducted using the STATinMED RWD Insights all-payer medical and pharmacy data. Adult patients with at least 1 CD medical claim and at least 1 medical/pharmacy claim for a biologic (adalimumab [ADA], certolizumab pegol (CZP), infliximab [IFX] and its biosimilar products [IFX-BS], ustekinumab [UST], and vedolizumab [VDZ]) between September 2016 and October 2018 were identified. Commercially insured patients with continuous capture for at least 12 months before and at least 36 months after biologics initiation were selected. Confirmed CD patients were included in the final cohort. Baseline patient characteristics and treatment patterns over the 3-year follow-up period were evaluated. Results were summarized using means and SD or counts and percentages. Results: A total of 2309 confirmed patients with CD were identified (847 [36.7%] IFX, 534 [23.1%] ADA, 486 [21.1%] VDZ, 394 [17.1%] UST, 85 [3.7%] CZP, and 72 [3.1%] IFX-BS). CZP and IFX-BS were excluded due to small sample sizes. Approximately half of CD patients were between ages 35 and 54. Patients on UST had a higher Charlson Comorbidity Index score. Common comorbidities (>10%) included anemia, anxiety, depression, and hypertension. Persistence over 3 years' follow-up was highest for UST (61.4%) patients, followed by VDZ (58.0% ), ADA (52.1% , and IFX (48.1%). The discontinuation rate without switch or restart was highest for ADA (37.3%), followed by UST (30.7%), IFX (28.1%), and VDZ (25.3%). Over the 3 years of follow-up, the dose titration rate was highest for IFX (76.5%) and lowest for UST (50.8%). In particular, UST had the lowest dose escalation rate (35.5%) and highest dose-reduction rate (16.5%). Conclusions: Patients with CD on UST had the highest persistence and lowest dose escalation across different biologic users over the 3-year follow-up period, possibly suggesting a better clinical response of UST. Future studies with longer follow-up adjusting for confounders are needed to better understand treatment patterns among biologics users.

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