| Literature DB >> 33741584 |
Thales Antonio Cabral de Guimaraes1,2, Malena Daich Varela1,2, Michalis Georgiou1,2, Michel Michaelides3,2.
Abstract
Age-related macular degeneration (AMD) is the leading cause of irreversible blindness in the developed world. The identification of the central role of vascular endothelial growth factor (VEGF) in the pathogenesis of neovascular AMD and the introduction of anti-VEGF agents as gold-standard treatment, have drastically changed its prognosis-something yet to be seen in dry AMD. Several therapeutic avenues with a wide variability of targets are currently being investigated in dry AMD. The approaches being investigated to reduce the rate of disease progression include, (1) drugs with antioxidative properties, (2) inhibitors of the complement cascade, (3) neuroprotective agents, (4) visual cycle inhibitors, (5) gene therapy and (6) cell-based therapies. A number of early phase clinical trials have provided promising results, with many more ongoing and anticipated in the near future. In this review, we aim to provide an update of the interventional trials to date and future prospects for the treatment of dry AMD. © Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY. Published by BMJ.Entities:
Keywords: angiogenesis; degeneration; genetics; macula; retina
Mesh:
Substances:
Year: 2021 PMID: 33741584 PMCID: PMC8867261 DOI: 10.1136/bjophthalmol-2020-318452
Source DB: PubMed Journal: Br J Ophthalmol ISSN: 0007-1161 Impact factor: 4.638
Summary of ongoing clinical trials targeting dry AMD
| Drug category/name | Clinical trial ID (NCT #) | Study phase | Route of delivery | Status | Sponsor | Location | Number of patients |
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| AREDS | NCT00000145 | Phase III | Oral | Completed | National Eye Institute (NEI) | USA | 3640 |
| AREDS2 | NCT00345176 | Phase III | Oral | Completed | National Eye Institute (NEI) | USA | 4203 |
| OT-551 | NCT00306488 | Phase II | Topical | Completed | National Institutes of Health Clinical Center (CC) | USA | 11 |
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| GSK933776 | NCT01342926 | Phase II | IV | Completed | GlaxoSmithKline | USA | 191 |
| RN6G | NCT01577381 | Phase II | IV | Terminated | Pfizer | USA | 10 |
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| ACU-4429 | NCT01802866 | Phase IIb/III | Oral | Completed | Kutoba Vision Inc | USA | 508 |
| Fenretinide | NCT00429936 | Phase II | Oral | Completed | Sirion Therapeutics, Inc | USA | 246 |
| C20-D3-vitamin A (ALK-001) | NCT03845582 | Phase III | Oral | Ongoing—recruiting | Alkeus Pharmaceuticals, Inc | USA | 300 |
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| Eculizumab | NCT00935883 | Phase II | IV | Completed | Philip J. Rosenfeld, MD | USA | 30 |
| Lampalizumab | NCT02247531 | Phase III | Intravitreal | Terminated | Hoffman-La Roche | Multicenter | 906 |
| Lampalizumab | NCT02247479 | Phase III | Intravitreal | Terminated | Hoffman-La Roche | Multicenter | 975 |
| Sirolimus (rapamycin) | NCT00766649 | Phase I/II | Subconjunctival | Completed | National Eye Institute (NEI) | USA | 11 |
| Avacincaptad pegol (Zimura) | NCT02686658 | Phase II/III | Intravitreal | Completed | IVERIC bio, Inc. | Multicenter | 286 |
| Pegcetacoplan (APL-2) | NCT02503332 | Phase II | Intravitreal | Completed | Apellis Pharmaceuticals Inc. | Multicenter | 246 |
| Pegcetacoplan (APL-2) | NCT03525600 | Phase III | Intravitreal | Ongoing—not recruiting | Apellis Pharmaceuticals Inc. | Multicenter | 600 |
| Pegcetacoplan (APL-2) | NCT03525613 | Phase III | Intravitreal | Ongoing—not recruiting | Apellis Pharmaceuticals Inc. | Multicenter | 600 |
| Tedisolumab (LFG316) | NCT01527500 | Phase II | Intravitreal | Completed | Novartis Pharmaceuticals | USA | 150 |
| Risuteganib | NCT03626636 | Phase II | Intravitreal | Completed | Allegro Ophthalmics | USA | 42 |
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| Ciliary nerve trophic factor | NCT00063765 | Phase I | Intravitreal | Completed | National Eye Institute (NEI) | USA | 10 |
| Ciliary nerve trophic factor | NCT00447954 | Phase II | Intravitreal | Completed | Neurotech Pharmaceuticals | USA | 51 |
| Brimonidine tartrate | NCT00658619 | Phase II | Intravitreal | Completed | Allergan | Multicenter | 113 |
| Brimonidine tartrate | NCT02087085 | Phase IIb | Intravitreal | Terminated | Allergan | Multicenter | 303 |
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| AAVCAGsCD59 | NCT03144999 | Phase I | Intravitreal | Completed | Hemera Biosciences | USA | 17 |
| GT005 | NCT03846193 | Phase I/II | Subretinal | Ongoing - Recruiting | Gyroscope Therapeutics | UK | 35 |
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| Palucorcel (CNTO-2476) | NCT01226628 | Phase I/II | Subretinal | Completed | Janssen Research & Development, LLC | USA | 35 |
| MA09-hRPE | NCT01344993 | Phase I/II | Subretinal | Completed | Astelas Institute for Regenerative Medicine | USA | 9 |
| CPCB-RPE1 | NCT02590692 | Phase I/IIa | Subretinal | Ongoing—not recruiting | Regenerative Patch Technologies | USA | 16 |
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| Elamipretide | NCT02848313 | Phase I | Subcutaneous | Completed | Stealth Biotechnologies Inc | USA | 40 |
| Elamipretide | NCT03891875 | Phase II | Subcutaneous | Ongoing—recruiting | Stealth Biotechnologies Inc | USA | 180 |
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| 2RT nanosecond laser | NCT01790802 | Not applicable | Retinal active laser therapy | Completed | Center for Eye Research Australia | Australia | 292 |
AMD, age-related macular degeneration.
Figure 1Graphical representation of the complement cascade. The location where different therapeutics act is highlighted. The therapies are shown, with them all have a downregulating effect on the particular step, negatively impacting on the downstream pathway. This figure has been created by the authors. C, complement; IgG, immunoglobulin G; MAC, membrane attack complex.