Real-world prevalence of potential drug-drug interactions associated with oral advanced therapies indicated for ulcerative colitis.

IF 2.4 4区医学 Q1 MEDICINE, GENERAL & INTERNAL

Current Medical Research and Opinion Pub Date : 2025-02-01 Epub Date: 2025-02-28 DOI:10.1080/03007995.2025.2465649

Maryia Zhdanava, Sabree Burbage, Todor I Totev, Sumesh Kachroo, Lilian Diaz, Bridget Godwin, Patrick Lefebvre, Dominic Pilon

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引用次数: 0

Abstract

Objective: To describe potential drug-drug interactions (DDIs) with oral advanced therapies among patients with ulcerative colitis (UC) and characterize clinical assessments before ozanimod initiation.

Methods: Adults with UC were selected from the Merative MarketScan Commercial Database (01 January 2018-31 January 2023); the index date was the most recent UC diagnosis. Patients had no other immune conditions in the 12-month baseline period before the index date. Those with moderate-to-severe UC were analyzed separately. Potential baseline DDIs were identified as claims for medications that may cause a moderate/severe DDI with Janus kinase (JAK) inhibitors (tofacitinib/upadacitinib) or ozanimod according to the Merative Micromedex Complete Drug Interactions Tool. Clinical assessments before ozanimod initiation were characterized.

Results: Of 58,870 patients with UC, 24,654 (41.9%) had moderate-to-severe UC. All potential DDIs with ozanimod were severe, while JAK inhibitors had moderate and severe potential DDIs. Among patients with UC, mean (standard deviation) number of severe DDIs was 2.0 (2.4) for ozanimod and 0.2 (0.5) for JAK inhibitors; in moderate-to-severe UC, it was 2.3 (2.6) for ozanimod and 0.4 (0.6) for JAK inhibitors. The most common potential DDIs for ozanimod in UC and moderate-to-severe UC were ondansetron (18.6% and 22.7%), azithromycin (11.9% and 12.8%), as well as hydrocodone, fentanyl, albuterol, ciprofloxacin, and metronidazole (9.0%-11.0% each). For JAK inhibitors, these were COVID-19 vaccines (30.7% and 31.4%), infliximab (8.5% and 20.2%), fluconazole (6.1% and 6.8%), and azathioprine (5.5% and 13.0%). Among patients initiating ozanimod, the first claim for a required clinical assessment was on average, 8 months before initiation.

Conclusion: Comorbidities and polypharmacy among patients with UC pose a high risk of DDIs for oral advanced therapies and required pre-treatment clinical assessments can be complicated. This justifies a thorough review of patient profiles for prescribers considering novel treatment options.

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与溃疡性结肠炎的口服高级疗法相关的潜在药物-药物相互作用的现实患病率。

目的：描述溃疡性结肠炎（UC）患者口服高级疗法的潜在药物-药物相互作用（ddi），并描述ozanimod开始前的临床评估特征。方法：从Merative™MarketScan®商业数据库（2018年1月1日- 2023年1月31日）中选择患有UC的成人；索引日期为最近的UC诊断。在索引日期前的12个月基线期内，患者没有其他免疫疾病。中度至重度UC患者分别进行分析。根据Merative™Micromedex®完全药物相互作用工具，潜在基线DDI被确定为可能导致Janus激酶（JAK）抑制剂（tofacitinib/upadacitinib）或ozanimod的中度/重度DDI的药物声明。在ozanimod开始前进行临床评估。结果：58,870例UC患者中，24,654例（41.9%）为中度至重度UC。ozanimod的所有潜在ddi都是严重的，而JAK抑制剂的潜在ddi是中度和重度的。在UC患者中，ozanimod组严重ddi的平均（标准差）数为2.0 (2.4)，JAK抑制剂组为0.2 (0.5)；在中重度UC中，ozanimod为2.3 (2.6)，JAK抑制剂为0.4（0.6）。ozanimod在UC和中重度UC中最常见的潜在ddi是昂丹西琼（18.6%和22.7%）、阿奇霉素（11.9%和12.8%），以及氢可酮、芬太尼、沙丁胺醇、环丙沙星和甲硝唑（9.0%-11.0%）。对于JAK抑制剂，这些是COVID-19疫苗（30.7%和31.4%），英夫利昔单抗（8.5%和20.2%），氟康唑（6.1%和6.8%）和硫唑嘌呤（5.5%和13.0%）。在开始使用ozanimod的患者中，首次要求进行必要的临床评估的平均时间是在开始使用前8个月。结论：UC患者的合并症和多重用药构成了口服高级治疗ddi的高风险，且所需的治疗前临床评估可能比较复杂。这证明了医生在考虑新的治疗方案时对患者资料进行全面审查是合理的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Current Medical Research and Opinion 医学-医学：内科

CiteScore

4.40

自引率

4.30%

发文量

247

审稿时长

3-8 weeks

期刊介绍： Current Medical Research and Opinion is a MEDLINE-indexed, peer-reviewed, international journal for the rapid publication of original research on new and existing drugs and therapies, Phase II-IV studies, and post-marketing investigations. Equivalence, safety and efficacy/effectiveness studies are especially encouraged. Preclinical, Phase I, pharmacoeconomic, outcomes and quality of life studies may also be considered if there is clear clinical relevance