在体注射用利纳西珠单抗治疗中重度克罗恩病的疗效、安全性、患者体验和耐受性。
Efficacy, Safety, Patient Experience, and Tolerability of Risankizumab Administered by On-Body Injector for Moderate to Severe Crohn's Disease.
机构信息
Mayo Clinic College of Medicine and Science, Rochester, MN, USA.
AbbVie Inc, North Chicago, IL, USA.
出版信息
Adv Ther. 2023 May;40(5):2311-2325. doi: 10.1007/s12325-023-02477-2. Epub 2023 Mar 14.
INTRODUCTION
In patients with moderate to severe Crohn's disease (CD), intravenous induction and subcutaneous maintenance dosing with risankizumab was efficacious and well tolerated. Long-term management of CD via self-administration of risankizumab using an on-body injector (OBI) may improve treatment adherence through convenience and ease of use.
METHODS
Within the FORTIFY maintenance study, 46 patients from the United States (US) sites participated in an open-label extension Substudy and received 180 mg or 360 mg risankizumab delivered subcutaneously via OBI [360 mg (2.4 mL, 150 mg/mL) or 180 mg (1.2 mL, 150 mg/mL)]. At the Week 0 visit, patients were trained (pre-injection) by site staff, using Instructions for Use (IFU) and a training video, to self-administer risankizumab at Weeks 0 (on site), 8 (at home), and 16 (on site). Key objectives of the Substudy 4 were to assess OBI usability (observer rating of successful self-administration), hazard-free self-injection at Weeks 0 and 16, and patient rating of acceptability using the Self-Injection Assessment Questionnaire (SIAQ) at Weeks 0, 8, and 16. Additionally, the proportion of patients in clinical remission (CD Activity Index < 150) was collected at Weeks 0 and 16.
RESULTS
All patients successfully self-administered risankizumab via OBI, including two patients who successfully self-administered with a second OBI (i.e., required two injection attempts). Acceptability of self-injection was high. Two patients (n = 2) experienced a use-related hazard. Stable clinical remission was observed with both risankizumab doses. Two patients experienced injection site reactions; neither was related to the OBI per investigator's assessment. Two device-related adverse events related to topical adhesive reactions were reported, both mild and resolved. No new safety risks were observed.
CONCLUSION
The efficacy and safety of maintenance risankizumab delivered via OBI and OBI usability support the use of this device in patients with moderate to severe CD.
TRIAL REGISTRATION
ClinicalTrials.gov identifiers NCT03105102 (FORTIFY).
介绍
在中重度克罗恩病(CD)患者中,静脉诱导和皮下维持剂量的 risankizumab 是有效且耐受良好的。通过使用体腔注射(OBI)进行 risankizumab 的自我给药,可能会通过便利性和易用性来改善 CD 的长期管理。
方法
在 FORTIFY 维持研究中,来自美国(US)站点的 46 名患者参加了开放标签扩展子研究,并接受了 180mg 或 360mg risankizumab 通过 OBI 皮下给药[360mg(2.4mL,150mg/mL)或 180mg(1.2mL,150mg/mL)]。在第 0 周就诊时,患者由现场工作人员根据使用说明(IFU)和培训视频进行培训,以便在第 0 周(现场)、第 8 周(在家)和第 16 周(现场)进行 risankizumab 的自我给药。子研究 4 的主要目标是评估 OBI 的可用性(观察者对成功自我给药的评估)、第 0 周和第 16 周无危险的自我注射以及第 0、8 和 16 周使用自我注射评估问卷(SIAQ)的患者可接受性。此外,还在第 0 周和第 16 周收集了临床缓解(CD 活动指数<150)患者的比例。
结果
所有患者均通过 OBI 成功进行了 risankizumab 的自我给药,包括两名成功使用第二支 OBI 进行自我给药的患者(即需要两次注射尝试)。自我注射的可接受性很高。两名患者(n=2)经历了与使用相关的危害。两种剂量的 risankizumab 均观察到稳定的临床缓解。两名患者出现注射部位反应;根据研究者的评估,均与 OBI 无关。报告了两例与设备相关的不良事件,均与局部粘性反应相关,均为轻度且已解决。未观察到新的安全风险。
结论
通过 OBI 给药的维持性 risankizumab 的疗效和安全性以及 OBI 的可用性支持在中重度 CD 患者中使用该设备。
试验注册
ClinicalTrials.gov 标识符 NCT03105102(FORTIFY)。
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