乌布格列净与降钙素基因相关肽靶向单克隆抗体偏头痛预防药物联合使用时的药代动力学和安全性:一项随机、1b 期药物相互作用研究。
Pharmacokinetics and safety of ubrogepant when coadministered with calcitonin gene-related peptide-targeted monoclonal antibody migraine preventives in participants with migraine: A randomized phase 1b drug-drug interaction study.
机构信息
Clinical Pharmacology, AbbVie, Madison, NJ, USA.
Headache Center of Southern California, Carlsbad, CA, USA.
出版信息
Headache. 2021 Apr;61(4):642-652. doi: 10.1111/head.14095. Epub 2021 Apr 5.
OBJECTIVE
To evaluate the impact of two calcitonin gene-related peptide (CGRP)-targeted monoclonal antibodies (mAbs), erenumab and galcanezumab, on the pharmacokinetic (PK) profile, safety, and tolerability of ubrogepant.
BACKGROUND
People taking CGRP-targeted mAbs for migraine prevention sometimes take ubrogepant, an oral small-molecule CGRP receptor antagonist, for acute treatment of breakthrough migraine attacks.
DESIGN
In this two-arm, multicenter, open-label, phase 1b trial, adults with migraine were randomized to arm 1 (ubrogepant ± erenumab) or arm 2 (ubrogepant ± galcanezumab). The PK profile of ubrogepant was characterized for administration before and 4 days after CGRP-targeted mAb injection. Participants received single-dose ubrogepant 100 mg on day 1, subcutaneous erenumab 140 mg (arm 1) or galcanezumab 240 mg (arm 2) on day 8, and ubrogepant 100 mg once daily on days 12-15. In each study arm, serial blood samples were drawn on days 1 and 12 for measurement of plasma ubrogepant concentrations. The primary outcomes were area under the plasma ubrogepant concentration-time curve (AUC) from time 0 to t post-dose (AUC ) and from time 0 to infinity (AUC ), and maximum plasma concentration (C ) of ubrogepant when ubrogepant was administered before or after a single dose of erenumab or galcanezumab. Vital signs and laboratory parameters were monitored.
RESULTS
Forty participants enrolled (20 per arm; mean [standard deviation] ages, 32.2 [8.9] and 38.4 [8.8] years; 50% [10/20] and 60% [12/20] female in arms 1 and 2, respectively). There were no significant differences in ubrogepant C after versus before erenumab administration (geometric least-squares mean [LSM] ratio, 1.04 [90% CI, 0.93-1.16]), and no significant differences in AUC (1.06 [0.96-1.16]) or AUC (1.05 [0.96-1.15]). Similarly, ubrogepant C (1.00 [90% CI, 0.82-1.20]), AUC (1.05 [0.90-1.23]), and AUC (1.05 [0.90-1.22]) geometric LSM ratios were statistically equivalent after galcanezumab versus ubrogepant alone. Treatment-emergent adverse events (TEAEs) were similar to those reported with each treatment alone. No serious TEAEs, TEAEs leading to discontinuation, or clinically relevant changes in laboratory parameters or vital signs were reported.
CONCLUSIONS
The PK profile of ubrogepant was not significantly changed and no safety concerns were identified when ubrogepant was coadministered with erenumab or galcanezumab.
目的
评估两种降钙素基因相关肽(CGRP)靶向单克隆抗体(mAb),依瑞奈珠单抗和加兰他敏,对乌布罗肽的药代动力学(PK)特征、安全性和耐受性的影响。
背景
预防偏头痛时使用 CGRP 靶向 mAb 的人群有时会使用乌布罗肽,一种口服小分子 CGRP 受体拮抗剂,用于急性治疗突破性偏头痛发作。
设计
在这项两臂、多中心、开放标签、1b 期试验中,偏头痛患者被随机分配至第 1 臂(乌布罗肽+依瑞奈珠单抗)或第 2 臂(乌布罗肽+加兰他敏)。在 CGRP 靶向 mAb 注射前和 4 天后,对乌布罗肽的 PK 特征进行了描述。第 1 天给予单剂量乌布罗肽 100mg,第 8 天给予依瑞奈珠单抗 140mg(第 1 臂)或加兰他敏 240mg(第 2 臂),第 12-15 天给予乌布罗肽 100mg 每日 1 次。在每个研究臂中,在第 1 天和第 12 天采集连续血样,以测量血浆乌布罗肽浓度。主要结局是乌布罗肽在接受依瑞奈珠单抗或加兰他敏单次剂量前后的血浆乌布罗肽浓度-时间曲线下面积(AUC)(AUC )和从时间 0 到无穷大(AUC ),以及乌布罗肽的最大血浆浓度(C )。监测生命体征和实验室参数。
结果
共有 40 名参与者入组(每组 20 名;平均[标准差]年龄分别为 32.2[8.9]和 38.4[8.8]岁;第 1 臂和第 2 臂中分别有 50%[10/20]和 60%[12/20]为女性)。与依瑞奈珠单抗给药前相比,乌布罗肽给药后 C 没有显著差异(几何最小二乘均值[LSM]比值为 1.04[90%置信区间,0.93-1.16]),AUC (1.06[0.96-1.16])或 AUC (1.05[0.96-1.15])也没有显著差异。同样,与乌布罗肽单药治疗相比,加兰他敏给药后乌布罗肽 C (1.00[90%置信区间,0.82-1.20])、AUC (1.05[0.90-1.23])和 AUC (1.05[0.90-1.22])的几何 LSM 比值均具有统计学等效性。治疗出现的不良事件(TEAE)与每种治疗单独报告的不良事件相似。未报告严重的 TEAEs、导致停药的 TEAEs 或临床相关的实验室参数或生命体征变化。
结论
当乌布罗肽与依瑞奈珠单抗或加兰他敏联合使用时,乌布罗肽的 PK 特征没有显著改变,也没有发现安全性问题。
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