TY - JOUR
T1 - Phase 3, Randomized, 20-Month Study of the Efficacy and Safety of Bimatoprost Implant in Patients with Open-Angle Glaucoma and Ocular Hypertension (ARTEMIS 2)
AU - the ARTEMIS 2 Study Group
AU - Bacharach, Jason
AU - Tatham, Andrew
AU - Ferguson, Gloria
AU - Belalcázar, Sandra
AU - Thieme, Hagen
AU - Goodkin, Margot L.
AU - Chen, Michelle Y.
AU - Guo, Qiang
AU - Liu, Jeen
AU - Robinson, Michael R.
AU - Bejanian, Marina
AU - Wirta, David L.
AU - Alezzandrini, Arturo
AU - Bercovich, Gabriel
AU - Deromedis, Pablo
AU - Furno Sola, Federico
AU - Gentile, Carolina
AU - Lerner, Simon
AU - Lupinacci, Anahi
AU - Zeolite, Carlos
AU - Birt, Catherine
AU - Crichton, Andrew
AU - Gagne, Sebastien
AU - Giunta, Michael
AU - Harasymowycz, Paul
AU - Jinapriya, Delan
AU - Nicolela, Marcelo
AU - Nixon, Donald
AU - Saurel, Patrick
AU - Yan, David
AU - Yuen, Darana
AU - Arango, Santiago
AU - Martinez, Alexander
AU - Parra Restrepo, Juan Camilo
AU - Korda, Vladimir
AU - Kadlecova, Jana
AU - Svacinova, Jitka
AU - Khairy, Hany
AU - El Ibiary, Hani
AU - El Sanabary, Zeinab
AU - Bell, Katharina
AU - Greslechner, Roman
AU - Koch, Jöerg
AU - Lorenz, Katrin
AU - Oberacher-Velten, Isabel
AU - Schmickler, Stefanie
AU - Schuart, Claudie
AU - Bandello, Francesco
AU - Cagini, Carlos
AU - Vizzeri, Gianmarco
N1 - Publisher Copyright:
© 2021, The Author(s).
PY - 2021/11
Y1 - 2021/11
N2 - Objective: To evaluate the intraocular pressure (IOP)-lowering efficacy and safety of 10 and 15 µg bimatoprost implant in patients with open-angle glaucoma (OAG) or ocular hypertension (OHT). Methods: This randomized, 20-month, multicenter, masked, parallel-group, phase 3 trial enrolled 528 patients with OAG or OHT and an open iridocorneal angle inferiorly in the study eye. Study eyes were administered 10 or 15 µg bimatoprost implant on day 1, week 16, and week 32, or twice-daily topical timolol maleate 0.5%. Primary endpoints were IOP and IOP change from baseline through week 12. Safety measures included treatment-emergent adverse events (TEAEs) and corneal endothelial cell density (CECD). Results: Both 10 and 15 µg bimatoprost implant met the primary endpoint of noninferiority to timolol in IOP lowering through 12 weeks. Mean IOP reductions from baseline ranged from 6.2–7.4, 6.5–7.8, and 6.1–6.7 mmHg through week 12 in the 10 µg implant, 15 µg implant, and timolol groups, respectively. IOP lowering was similar after the second and third implant administrations. Probabilities of requiring no IOP-lowering treatment for 1 year after the third administration were 77.5% (10 µg implant) and 79.0% (15 µg implant). The most common TEAE was conjunctival hyperemia, typically temporally associated with the administration procedure. Corneal TEAEs of interest (primarily corneal endothelial cell loss, corneal edema, and corneal touch) were more frequent with the 15 than the 10 µg implant and generally were reported after repeated administrations. Loss in mean CECD from baseline to month 20 was ~ 5% in 10 µg implant-treated eyes and ~ 1% in topical timolol-treated eyes. Visual field progression (change in the mean deviation from baseline) was reduced in the 10 µg implant group compared with the timolol group. Conclusions: The results corroborated the previous phase 3 study of the bimatoprost implant. The bimatoprost implant met the primary endpoint and effectively lowered IOP. The majority of patients required no additional treatment for 12 months after the third administration. The benefit-risk assessment favored the 10 over the 15 µg implant. Studies evaluating other administration regimens with reduced risk of corneal events are ongoing. The bimatoprost implant has the potential to improve adherence and reduce treatment burden in glaucoma. Clinicaltrials.gov Identifier: NCT02250651.
AB - Objective: To evaluate the intraocular pressure (IOP)-lowering efficacy and safety of 10 and 15 µg bimatoprost implant in patients with open-angle glaucoma (OAG) or ocular hypertension (OHT). Methods: This randomized, 20-month, multicenter, masked, parallel-group, phase 3 trial enrolled 528 patients with OAG or OHT and an open iridocorneal angle inferiorly in the study eye. Study eyes were administered 10 or 15 µg bimatoprost implant on day 1, week 16, and week 32, or twice-daily topical timolol maleate 0.5%. Primary endpoints were IOP and IOP change from baseline through week 12. Safety measures included treatment-emergent adverse events (TEAEs) and corneal endothelial cell density (CECD). Results: Both 10 and 15 µg bimatoprost implant met the primary endpoint of noninferiority to timolol in IOP lowering through 12 weeks. Mean IOP reductions from baseline ranged from 6.2–7.4, 6.5–7.8, and 6.1–6.7 mmHg through week 12 in the 10 µg implant, 15 µg implant, and timolol groups, respectively. IOP lowering was similar after the second and third implant administrations. Probabilities of requiring no IOP-lowering treatment for 1 year after the third administration were 77.5% (10 µg implant) and 79.0% (15 µg implant). The most common TEAE was conjunctival hyperemia, typically temporally associated with the administration procedure. Corneal TEAEs of interest (primarily corneal endothelial cell loss, corneal edema, and corneal touch) were more frequent with the 15 than the 10 µg implant and generally were reported after repeated administrations. Loss in mean CECD from baseline to month 20 was ~ 5% in 10 µg implant-treated eyes and ~ 1% in topical timolol-treated eyes. Visual field progression (change in the mean deviation from baseline) was reduced in the 10 µg implant group compared with the timolol group. Conclusions: The results corroborated the previous phase 3 study of the bimatoprost implant. The bimatoprost implant met the primary endpoint and effectively lowered IOP. The majority of patients required no additional treatment for 12 months after the third administration. The benefit-risk assessment favored the 10 over the 15 µg implant. Studies evaluating other administration regimens with reduced risk of corneal events are ongoing. The bimatoprost implant has the potential to improve adherence and reduce treatment burden in glaucoma. Clinicaltrials.gov Identifier: NCT02250651.
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U2 - 10.1007/s40265-021-01624-9
DO - 10.1007/s40265-021-01624-9
M3 - Article
C2 - 34724172
AN - SCOPUS:85118391493
SN - 0012-6667
VL - 81
SP - 2017
EP - 2033
JO - Drugs
JF - Drugs
IS - 17
ER -