Sarkisian Steven R, Ang Robert E, Lee Andy M, Berdahl John P, Heersink Sebastian B, Burden James H, Doan Long V, Stephens Kerry G, Applegate David, Kothe Angela C, Usner Dale W, Katz L Jay, Navratil Tomas
Oklahoma Eye Surgeons, PLLC, 5600 N Portland Avenue, Oklahoma City, OK, 73112, USA.
Asian Eye Institute, 8th to 10th Floor, Rockwell Center, PHINMA Plaza Building, 01200, Makati City, Philippines.
Ophthalmol Ther. 2024 Apr;13(4):995-1014. doi: 10.1007/s40123-024-00898-y. Epub 2024 Feb 12.
This prospective, multicenter, randomized, double-masked pivotal phase 3 trial evaluated the efficacy and safety of the travoprost intracameral SE-implant (slow-eluting implant, the intended commercial product) and FE-implant (fast-eluting implant, included primarily for masking purposes) compared to twice-daily (BID) timolol ophthalmic solution, 0.5% in patients with open-angle glaucoma (OAG) or ocular hypertension (OHT).
The trial enrolled adult patients with OAG or OHT with an unmedicated mean diurnal intraocular pressure (IOP) of ≥ 21 and unmedicated IOP ≤ 36 mmHg at each diurnal timepoint (8 A.M., 10 A.M., and 4 P.M.) at baseline. The eligible eye of each patient was administered an SE-implant, an FE-implant or had a sham administration procedure. Patients who received an implant were provided placebo eye drops to be administered BID and patients who had the sham procedure were provided timolol eye drops to be administered BID. The primary efficacy endpoint, for which the study was powered, was mean change from baseline IOP at 8 A.M. and 10 A.M. at day 10, week 6, and month 3. Non-inferiority was achieved if the upper 95% confidence interval (CI) on the difference in IOP change from baseline (implant minus timolol) was < 1.5 mmHg at all six timepoints and < 1 mmHg at three or more timepoints. The key secondary endpoint was mean change from baseline IOP at 8 A.M. and 10 A.M. at month 12. Non-inferiority at month 12 was achieved if the upper 95% CI was < 1.5 mmHg at both timepoints. Safety outcomes included treatment-emergent adverse events (TEAEs) and ophthalmic assessments.
A total of 590 patients were enrolled at 45 sites and randomized to one of three treatment groups: 197 SE-implant (the intended commercial product), 200 FE-implant, and 193 timolol. The SE-implant was non-inferior to timolol eye drops in IOP lowering over the first 3 months, and was also non-inferior to timolol at months 6, 9, and 12. The FE-implant was non-inferior to timolol over the first 3 months, and also at months 6 and 9. Of those patients who were on glaucoma medication at screening, a significantly greater proportion of patients in the SE- and FE-implant groups (83.5% and 78.7%, respectively) compared to the timolol group (23.9%) were on fewer topical glaucoma medications at month 12 compared to screening (P < 0.0001, chi-square test). TEAEs, mostly mild, were reported in the study eyes of 39.5% of patients in the SE-implant group, 34.0% of patients in the FE-implant group and 20.1% of patients in the timolol group.
The SE-travoprost intracameral implant demonstrated non-inferiority to timolol over 12 months whereas the FE-implant demonstrated non-inferiority over 9 months. Both implant models were safe and effective in IOP lowering in patients with OAG or OHT.
ClinicalTrials.gov identifier, NCT03519386.
这项前瞻性、多中心、随机、双盲关键3期试验评估了曲伏前列素前房内缓释植入物(SE-植入物,预期商业产品)和快速释放植入物(FE-植入物,主要用于设盲目的)与0.5%噻吗洛尔滴眼液每日两次给药相比,在开角型青光眼(OAG)或高眼压症(OHT)患者中的疗效和安全性。
该试验纳入了OAG或OHT成年患者,这些患者在基线时每个日间时间点(上午8点、上午10点和下午4点)未用药时的平均日间眼压(IOP)≥21 mmHg且未用药时的IOP≤36 mmHg。每位患者的符合条件的眼睛接受SE-植入物、FE-植入物或假手术操作。接受植入物的患者给予安慰剂滴眼液每日两次给药,接受假手术的患者给予噻吗洛尔滴眼液每日两次给药。该研究的主要疗效终点是第10天、第6周和第3个月上午8点和上午10点时与基线IOP的平均变化。如果在所有六个时间点眼压变化(植入物减去噻吗洛尔)差异的95%置信区间(CI)上限< 1.5 mmHg且在三个或更多时间点< 1 mmHg,则达到非劣效性。关键次要终点是第12个月上午8点和上午10点时与基线IOP的平均变化。如果在两个时间点95% CI上限< 1.5 mmHg,则在第12个月达到非劣效性。安全性结局包括治疗中出现的不良事件(TEAE)和眼科评估。
共有5个45个中心的590名患者入组并随机分为三个治疗组之一:197例接受SE-植入物(预期商业产品),200例接受FE-植入物,193例接受噻吗洛尔治疗。SE-植入物在降低眼压方面在最初3个月内不劣于噻吗洛尔滴眼液,在第6、9和12个月时也不劣于噻吗洛尔。FE-植入物在最初3个月内不劣于噻吗洛尔,在第6和9个月时也是如此。在筛查时正在使用青光眼药物治疗的患者中,与噻吗洛尔组(23.9%)相比,SE-植入物组和FE-植入物组中在第12个月时使用局部青光眼药物少于筛查时的患者比例显著更高(分别为83.5%和78.7%)(P<0.0001,卡方检验)。SE-植入物组39.5%的患者、FE-植入物组34.0%的患者和噻吗洛尔组20.1%的患者在研究眼中报告了TEAE,大多数为轻度。
曲伏前列素前房内SE-植入物在12个月内显示出不劣于噻吗洛尔,而FE-植入物在9个月内显示出不劣于噻吗洛尔。两种植入物模型在降低OAG或OHT患者眼压方面均安全有效。
ClinicalTrials.gov标识符,NCT03519386 。
