Phase 3, Randomized, 20-Month Study of Bimatoprost Implant in Open-Angle Glaucoma and Ocular Hypertension (ARTEMIS 1)

ARTEMIS 1 Study Group

doi:10.1016/j.ophtha.2020.06.018

Phase 3, Randomized, 20-Month Study of Bimatoprost Implant in Open-Angle Glaucoma and Ocular Hypertension (ARTEMIS 1)

ARTEMIS 1 Study Group

Ophthalmology & Visual Sciences

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48 Scopus citations

Abstract

Purpose: To evaluate the intraocular pressure (IOP)-lowering efficacy and safety of 10- and 15-μg bimatoprost implant in subjects with open-angle glaucoma (OAG) and ocular hypertension (OHT) after initial and repeated administrations. Design: Randomized, 20-month, multicenter, subject- and efficacy evaluator-masked, parallel-group, phase 3 clinical study. Participants: Adults with OAG or OHT in each eye, open iridocorneal angle inferiorly in the study eye, and study eye baseline IOP (hour 0; 8 AM) of 22–32 mmHg after washout. Methods: Study eyes received bimatoprost implant 10 μg (n = 198) or 15 μg (n = 198) on day 1 with readministration at weeks 16 and 32, or twice-daily topical timolol maleate 0.5% (n = 198). Intraocular pressure was measured at hours 0 and 2 at each visit. Main Outcome Measures: Primary end points were IOP and change from baseline IOP through week 12. Safety measures included treatment-emergent adverse events (TEAEs) and corneal endothelial cell density (CECD). Results: Both dose strengths of bimatoprost implant were noninferior to timolol in IOP lowering after each administration. Mean diurnal IOP was 24.0, 24.2, and 23.9 mmHg at baseline and from 16.5–17.2, 16.5–17.0, and 17.1–17.5 mmHg through week 12 in the 10-μg implant, 15-μg implant, and timolol groups, respectively. The incidence of corneal and inflammatory TEAEs of interest (e.g., corneal endothelial cell loss, iritis) was higher with bimatoprost implant than timolol and highest with the 15-μg dose strength. Incidence of corneal TEAEs increased after repeated treatment; with 3 administrations at fixed 16-week intervals, incidence of ≥20% CECD loss was 10.2% (10-μg implant) and 21.8% (15-μg implant). Mean best-corrected visual acuity (BCVA) was stable; 3 implant-treated subjects with corneal TEAEs had >2-line BCVA loss at their last visit. Conclusions: Both dose strengths of bimatoprost implant met the primary end point of noninferiority to timolol through week 12. One year after 3 administrations, IOP was controlled in most subjects without additional treatment. The risk-benefit assessment favored the 10-μg implant over the 15-μg implant. Ongoing studies are evaluating other administration regimens to reduce the potential for CECD loss. The bimatoprost implant has potential to improve adherence and reduce treatment burden in glaucoma.

Original language	English (US)
Pages (from-to)	1627-1641
Number of pages	15
Journal	Ophthalmology
Volume	127
Issue number	12
DOIs	https://doi.org/10.1016/j.ophtha.2020.06.018
State	Published - Dec 2020

ASJC Scopus subject areas

Ophthalmology

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10.1016/j.ophtha.2020.06.018

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@article{2b8290077a604cc989ac5d607ddb9183,

title = "Phase 3, Randomized, 20-Month Study of Bimatoprost Implant in Open-Angle Glaucoma and Ocular Hypertension (ARTEMIS 1)",

abstract = "Purpose: To evaluate the intraocular pressure (IOP)-lowering efficacy and safety of 10- and 15-μg bimatoprost implant in subjects with open-angle glaucoma (OAG) and ocular hypertension (OHT) after initial and repeated administrations. Design: Randomized, 20-month, multicenter, subject- and efficacy evaluator-masked, parallel-group, phase 3 clinical study. Participants: Adults with OAG or OHT in each eye, open iridocorneal angle inferiorly in the study eye, and study eye baseline IOP (hour 0; 8 AM) of 22–32 mmHg after washout. Methods: Study eyes received bimatoprost implant 10 μg (n = 198) or 15 μg (n = 198) on day 1 with readministration at weeks 16 and 32, or twice-daily topical timolol maleate 0.5% (n = 198). Intraocular pressure was measured at hours 0 and 2 at each visit. Main Outcome Measures: Primary end points were IOP and change from baseline IOP through week 12. Safety measures included treatment-emergent adverse events (TEAEs) and corneal endothelial cell density (CECD). Results: Both dose strengths of bimatoprost implant were noninferior to timolol in IOP lowering after each administration. Mean diurnal IOP was 24.0, 24.2, and 23.9 mmHg at baseline and from 16.5–17.2, 16.5–17.0, and 17.1–17.5 mmHg through week 12 in the 10-μg implant, 15-μg implant, and timolol groups, respectively. The incidence of corneal and inflammatory TEAEs of interest (e.g., corneal endothelial cell loss, iritis) was higher with bimatoprost implant than timolol and highest with the 15-μg dose strength. Incidence of corneal TEAEs increased after repeated treatment; with 3 administrations at fixed 16-week intervals, incidence of ≥20% CECD loss was 10.2% (10-μg implant) and 21.8% (15-μg implant). Mean best-corrected visual acuity (BCVA) was stable; 3 implant-treated subjects with corneal TEAEs had >2-line BCVA loss at their last visit. Conclusions: Both dose strengths of bimatoprost implant met the primary end point of noninferiority to timolol through week 12. One year after 3 administrations, IOP was controlled in most subjects without additional treatment. The risk-benefit assessment favored the 10-μg implant over the 15-μg implant. Ongoing studies are evaluating other administration regimens to reduce the potential for CECD loss. The bimatoprost implant has potential to improve adherence and reduce treatment burden in glaucoma.",

author = "{ARTEMIS 1 Study Group} and Medeiros, {Felipe A.} and Walters, {Thomas R.} and Miriam Kolko and Michael Coote and Marina Bejanian and Goodkin, {Margot L.} and Qiang Guo and Jane Zhang and Robinson, {Michael R.} and Weinreb, {Robert N.} and Ashish Agar and Renuka Bathijia and Lance Liu and Tim Roberts and Christoph Faschinger and Clemens Vass and Nathalie Collignon and {Alves Pereira}, {Ana Claudia} and {Belfort de Mattos}, Rubens and Dantas, {Fernando Justino} and {Lopes da Silva}, {Marcelo Jordao} and Fabio Kanadani and {Magacho dos Santos Silva}, Leopoldo and Tiago Prata and Daniella Bach-Holm and Jimmy Lai and Clement Tham and Gy{\"o}rgy B{\'a}tor and Lajos Szalczer and Bal{\'a}zs Vars{\'a}nyi and Eytan Blumenthal and Orna Geyer and Shmuel Lavartovsky and Tamar Pedut-Kloizman and Nir Shoham-Hazon and Silvio Lujan and Benjamin Abela and Ang, {Robert E.} and Leuenberger, {Edgar U.} and Harvey Uy and Yap-Veloso, {Maria Imelda} and Piotr Fryczkowski and Piotr Jurowski and Bartlomiej Kalu{\.z}ny and J{\'o}zef Kalu{\.z}ny and Marta Misiuk-Hojlo and Krystyna Raczynska and Wioletta Tomczyk-Dorozynska and Jaromir Wasyluk and Anurag Shrivastava",

note = "Funding Information: Kevin Wang, PhD, an independent contractor funded by Allergan plc, contributed to the statistical analyses for the manuscript under the direction of the authors. Adnan Salemeh, PhD, of Allergan plc (Irvine, CA), provided the in vitro drug release data, and Jennifer R. Seal, PhD, of Allergan plc (Irvine, CA), provided the animal pharmacokinetics data. Michele Jacob, PhD, of Evidence Scientific Solutions, Inc. (Philadelphia, PA), prepared a draft of the manuscript under the direction of the authors and provided editorial assistance, funded by Allergan plc. All authors met the International Committee of Medical Journal Editors authorship criteria. Neither honoraria nor payments were made for authorship. Funding Information: Financial Disclosure(s): The author(s) have made the following disclosure(s): F.A.M.: Consultant ? Allergan, Annexon, Aerie Pharmaceuticals, Biogen, Carl Zeiss Meditec, Galimedix, Novartis, Reichert, Stealth BioTherapeutics; Research support ? Carl Zeiss Meditec, Google, Heidelberg Engineering, Reichert; Founder ? NGoggle, Inc.M.K.: Consultant and speaker ? Allergan, Santen, Thea; Research support ? LeoPharma, Thea.R.N.W.: Consultant ? Aerie Pharmaceuticals, Allergan plc, Eyenovia, Galimedix, Implantdata, Novartis; Research support ? Bausch + Lomb, Centervue, Heidelberg Engineering, Konan, Meditec-Zeiss, National Eye Institute, Optovue; Founder ? Toromedes; Royalties ? University of California San Diego from Carl Zeiss Meditec.Sponsored by Allergan plc (Dublin, Ireland). The sponsor participated in the design of the study, data management, data analysis, interpretation of the data, and preparation, review, and approval of the manuscript. Obtained funding: N/A Publisher Copyright: {\textcopyright} 2020 American Academy of Ophthalmology",

year = "2020",

month = dec,

doi = "10.1016/j.ophtha.2020.06.018",

language = "English (US)",

volume = "127",

pages = "1627--1641",

journal = "Ophthalmology",

issn = "0161-6420",

publisher = "Elsevier Inc.",

number = "12",

}

TY - JOUR

T1 - Phase 3, Randomized, 20-Month Study of Bimatoprost Implant in Open-Angle Glaucoma and Ocular Hypertension (ARTEMIS 1)

AU - ARTEMIS 1 Study Group

AU - Medeiros, Felipe A.

AU - Walters, Thomas R.

AU - Kolko, Miriam

AU - Coote, Michael

AU - Bejanian, Marina

AU - Goodkin, Margot L.

AU - Guo, Qiang

AU - Zhang, Jane

AU - Robinson, Michael R.

AU - Weinreb, Robert N.

AU - Agar, Ashish

AU - Bathijia, Renuka

AU - Liu, Lance

AU - Roberts, Tim

AU - Faschinger, Christoph

AU - Vass, Clemens

AU - Collignon, Nathalie

AU - Alves Pereira, Ana Claudia

AU - Belfort de Mattos, Rubens

AU - Dantas, Fernando Justino

AU - Lopes da Silva, Marcelo Jordao

AU - Kanadani, Fabio

AU - Magacho dos Santos Silva, Leopoldo

AU - Prata, Tiago

AU - Bach-Holm, Daniella

AU - Lai, Jimmy

AU - Tham, Clement

AU - Bátor, György

AU - Szalczer, Lajos

AU - Varsányi, Balázs

AU - Blumenthal, Eytan

AU - Geyer, Orna

AU - Lavartovsky, Shmuel

AU - Pedut-Kloizman, Tamar

AU - Shoham-Hazon, Nir

AU - Lujan, Silvio

AU - Abela, Benjamin

AU - Ang, Robert E.

AU - Leuenberger, Edgar U.

AU - Uy, Harvey

AU - Yap-Veloso, Maria Imelda

AU - Fryczkowski, Piotr

AU - Jurowski, Piotr

AU - Kalużny, Bartlomiej

AU - Kalużny, Józef

AU - Misiuk-Hojlo, Marta

AU - Raczynska, Krystyna

AU - Tomczyk-Dorozynska, Wioletta

AU - Wasyluk, Jaromir

AU - Shrivastava, Anurag

N1 - Funding Information: Kevin Wang, PhD, an independent contractor funded by Allergan plc, contributed to the statistical analyses for the manuscript under the direction of the authors. Adnan Salemeh, PhD, of Allergan plc (Irvine, CA), provided the in vitro drug release data, and Jennifer R. Seal, PhD, of Allergan plc (Irvine, CA), provided the animal pharmacokinetics data. Michele Jacob, PhD, of Evidence Scientific Solutions, Inc. (Philadelphia, PA), prepared a draft of the manuscript under the direction of the authors and provided editorial assistance, funded by Allergan plc. All authors met the International Committee of Medical Journal Editors authorship criteria. Neither honoraria nor payments were made for authorship. Funding Information: Financial Disclosure(s): The author(s) have made the following disclosure(s): F.A.M.: Consultant ? Allergan, Annexon, Aerie Pharmaceuticals, Biogen, Carl Zeiss Meditec, Galimedix, Novartis, Reichert, Stealth BioTherapeutics; Research support ? Carl Zeiss Meditec, Google, Heidelberg Engineering, Reichert; Founder ? NGoggle, Inc.M.K.: Consultant and speaker ? Allergan, Santen, Thea; Research support ? LeoPharma, Thea.R.N.W.: Consultant ? Aerie Pharmaceuticals, Allergan plc, Eyenovia, Galimedix, Implantdata, Novartis; Research support ? Bausch + Lomb, Centervue, Heidelberg Engineering, Konan, Meditec-Zeiss, National Eye Institute, Optovue; Founder ? Toromedes; Royalties ? University of California San Diego from Carl Zeiss Meditec.Sponsored by Allergan plc (Dublin, Ireland). The sponsor participated in the design of the study, data management, data analysis, interpretation of the data, and preparation, review, and approval of the manuscript. Obtained funding: N/A Publisher Copyright: © 2020 American Academy of Ophthalmology

PY - 2020/12

Y1 - 2020/12

N2 - Purpose: To evaluate the intraocular pressure (IOP)-lowering efficacy and safety of 10- and 15-μg bimatoprost implant in subjects with open-angle glaucoma (OAG) and ocular hypertension (OHT) after initial and repeated administrations. Design: Randomized, 20-month, multicenter, subject- and efficacy evaluator-masked, parallel-group, phase 3 clinical study. Participants: Adults with OAG or OHT in each eye, open iridocorneal angle inferiorly in the study eye, and study eye baseline IOP (hour 0; 8 AM) of 22–32 mmHg after washout. Methods: Study eyes received bimatoprost implant 10 μg (n = 198) or 15 μg (n = 198) on day 1 with readministration at weeks 16 and 32, or twice-daily topical timolol maleate 0.5% (n = 198). Intraocular pressure was measured at hours 0 and 2 at each visit. Main Outcome Measures: Primary end points were IOP and change from baseline IOP through week 12. Safety measures included treatment-emergent adverse events (TEAEs) and corneal endothelial cell density (CECD). Results: Both dose strengths of bimatoprost implant were noninferior to timolol in IOP lowering after each administration. Mean diurnal IOP was 24.0, 24.2, and 23.9 mmHg at baseline and from 16.5–17.2, 16.5–17.0, and 17.1–17.5 mmHg through week 12 in the 10-μg implant, 15-μg implant, and timolol groups, respectively. The incidence of corneal and inflammatory TEAEs of interest (e.g., corneal endothelial cell loss, iritis) was higher with bimatoprost implant than timolol and highest with the 15-μg dose strength. Incidence of corneal TEAEs increased after repeated treatment; with 3 administrations at fixed 16-week intervals, incidence of ≥20% CECD loss was 10.2% (10-μg implant) and 21.8% (15-μg implant). Mean best-corrected visual acuity (BCVA) was stable; 3 implant-treated subjects with corneal TEAEs had >2-line BCVA loss at their last visit. Conclusions: Both dose strengths of bimatoprost implant met the primary end point of noninferiority to timolol through week 12. One year after 3 administrations, IOP was controlled in most subjects without additional treatment. The risk-benefit assessment favored the 10-μg implant over the 15-μg implant. Ongoing studies are evaluating other administration regimens to reduce the potential for CECD loss. The bimatoprost implant has potential to improve adherence and reduce treatment burden in glaucoma.

AB - Purpose: To evaluate the intraocular pressure (IOP)-lowering efficacy and safety of 10- and 15-μg bimatoprost implant in subjects with open-angle glaucoma (OAG) and ocular hypertension (OHT) after initial and repeated administrations. Design: Randomized, 20-month, multicenter, subject- and efficacy evaluator-masked, parallel-group, phase 3 clinical study. Participants: Adults with OAG or OHT in each eye, open iridocorneal angle inferiorly in the study eye, and study eye baseline IOP (hour 0; 8 AM) of 22–32 mmHg after washout. Methods: Study eyes received bimatoprost implant 10 μg (n = 198) or 15 μg (n = 198) on day 1 with readministration at weeks 16 and 32, or twice-daily topical timolol maleate 0.5% (n = 198). Intraocular pressure was measured at hours 0 and 2 at each visit. Main Outcome Measures: Primary end points were IOP and change from baseline IOP through week 12. Safety measures included treatment-emergent adverse events (TEAEs) and corneal endothelial cell density (CECD). Results: Both dose strengths of bimatoprost implant were noninferior to timolol in IOP lowering after each administration. Mean diurnal IOP was 24.0, 24.2, and 23.9 mmHg at baseline and from 16.5–17.2, 16.5–17.0, and 17.1–17.5 mmHg through week 12 in the 10-μg implant, 15-μg implant, and timolol groups, respectively. The incidence of corneal and inflammatory TEAEs of interest (e.g., corneal endothelial cell loss, iritis) was higher with bimatoprost implant than timolol and highest with the 15-μg dose strength. Incidence of corneal TEAEs increased after repeated treatment; with 3 administrations at fixed 16-week intervals, incidence of ≥20% CECD loss was 10.2% (10-μg implant) and 21.8% (15-μg implant). Mean best-corrected visual acuity (BCVA) was stable; 3 implant-treated subjects with corneal TEAEs had >2-line BCVA loss at their last visit. Conclusions: Both dose strengths of bimatoprost implant met the primary end point of noninferiority to timolol through week 12. One year after 3 administrations, IOP was controlled in most subjects without additional treatment. The risk-benefit assessment favored the 10-μg implant over the 15-μg implant. Ongoing studies are evaluating other administration regimens to reduce the potential for CECD loss. The bimatoprost implant has potential to improve adherence and reduce treatment burden in glaucoma.

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UR - http://www.scopus.com/inward/citedby.url?scp=85089012127&partnerID=8YFLogxK

U2 - 10.1016/j.ophtha.2020.06.018

DO - 10.1016/j.ophtha.2020.06.018

M3 - Article

C2 - 32544560

AN - SCOPUS:85089012127

SN - 0161-6420

VL - 127

SP - 1627

EP - 1641

JO - Ophthalmology

JF - Ophthalmology

IS - 12

ER -

Phase 3, Randomized, 20-Month Study of Bimatoprost Implant in Open-Angle Glaucoma and Ocular Hypertension (ARTEMIS 1)

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