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This is a multi-center, randomized, double-masked, active-comparator-controlled, Phase 3 study in a broad participant population (treatment-naïve and treatment-experienced) with neovascular (wet) age-related macular degeneration (nAMD). The study will evaluate a single intravitreal (IVT) injection of Ixo-vec compared to an active comparator. The primary endpoint of this study is the mean change in best corrected visual acuity (BCVA) of Ixo-vec compared to an active comparator measured at an average of Weeks 52 and 56.
Safety, tolerability, and efficacy will be evaluated throughout the study.
The primary objective of this study is to evaluate the non-inferiority in efficacy of a single intravitreal (IVT) injection of Ixo-vec 6 x 10^10 vector genome (vg)/eye compared to an active comparator.
Neovascular or wet age-related macular degeneration (nAMD) is a degenerative ocular disease associated with the infiltration of abnormal blood vessels in the retina from the underlying choroid layer and is a leading cause of blindness in patients over 65 years of age. The abnormal angiogenic process in nAMD is stimulated and modulated by vascular endothelial growth factor (VEGF). Treatment of nAMD requires frequent intravitreal (IVT) injections of VEGF inhibitors (anti-VEGF) administered every 4-16 weeks. Ixo-vec (also known as ADVM-022 or AAV.7m8-aflibercept) is a gene therapy product being developed for the treatment of nAMD. Ixo-vec is designed to reduce the current treatment burden which often results in undertreatment and vision loss in patients with nAMD receiving anti-VEGF therapy in clinical practice. This study will be considered fully enrolled when randomization has been completed.
Safety, tolerability, and efficacy will be evaluated throughout this study. The primary endpoint of this study is the mean change in best corrected visual acuity (BCVA) of Ixo-vec compared to an active comparator measured at an average of Weeks 52 and 56 post-treatment.
After completing the Week 56 visit, participants will continue in the long-term follow-up period for 4 additional years (a total of 5 years on study).
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Ixo-vec | Experimental | Participants will receive 3 monthly loading doses of aflibercept 2 mg IVT, a single IVT injection of Ixo-vec 6 x 10^10 vg/eye at Week 1, and sham injections every 8 weeks |
|
| Aflibercept | Active Comparator | Participants will receive 3 monthly loading doses of aflibercept 2 mg IVT, a sham injection at Week 1, and aflibercept 2 mg IVT every 8 weeks. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Ixo-vec | Genetic | Ixo-vec will be administered intravitreally. |
| |
| Measure | Description | Time Frame |
|---|---|---|
| Mean change from Baseline in Best-Corrected Visual Acuity (BCVA) based on an average at Weeks 52 and 56 | BCVA will be measured using an Early Treatment Diabetic Retinopathy Study (ETDRS) visual acuity chart. | Baseline, Week 52 and Week 56 |
| Measure | Description | Time Frame |
|---|---|---|
| Mean number of aflibercept IVT injections received | Week 4 through Week 56 | |
| Percentage of participants with worsened BCVA from Baseline through Week 56 and Week 104 | BCVA measured by ETDRS | Baseline through Week 56 and Week 104 |
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Inclusion Criteria:
Exclusion Criteria:
General Exclusion Criteria
History of a medical condition giving reasonable suspicion of a condition that contraindicates the use of Ixo-vec, compromises the participant's ability to comply with the planned study activities, or that might affect the interpretation of the results of the study or render the participant at high risk for treatment complications in the opinion of the Investigator. History of severe coronavirus disease (COVID-19) infection may meet this exclusion criteria if, in the opinion of the Investigator, it is likely to lead to any important complications.
Received any prior gene therapy.
Prior treatment with any non-gene therapy investigational medicinal product (IMP) or medical device in the study eye within 3 months of Screening Visit 1 or 5 half-lives of the IMP prior to dosing with Ixo-vec, whichever is longer.
Female participants who are pregnant or breastfeeding or who intend to become pregnant or breastfeed in the future.
History or evidence of any of the following cardiovascular diseases:
History of ongoing bleeding disorders. The use of aspirin or other anticoagulants (e.g., Factor Xa inhibitors) is permitted.
Use of systemic immunosuppressive drugs within 90 days prior to Screening Visit 1. Short courses of oral corticosteroids are permitted, as well as any inhaled, intra-articular, nasal or dermal steroid use.
Evidence of poorly controlled diabetes or glycated hemoglobin (HbA1c) ≥ 8.0% during screening
Ocular Exclusion Criteria
Any active ocular or periocular infection in the study eye from Screening Visit 1.
History or evidence of the following in the study eye:
Any history or evidence of retinal detachment (with or without repair) or retinal pigment epithelium rip/tear in the study eye, as determined by the Investigator during screening or at Week 1.
Uncontrolled ocular hypertension or glaucoma in the study eye from Screening Visit 1 to Week 1 or current use of ≥ 2 IOP lowering medications or normal tension glaucoma/suspect in the study eye or history of any of the following procedures in the study eye prior to Week 1:
Any history of intraocular pressure (IOP) elevation related to topical steroid administration in either eye.
Any history of uveitis or inflammation (grade trace or above) except mild anticipated post operative inflammation that resolved in either eye.
Any history of treatment with complement inhibitors for geographic atrophy in the study eye.
Known history of ocular herpes simplex virus, varicella-zoster virus, or cytomegalovirus, including viral uveitis, retinitis, or keratitis in either eye.
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| Name | Affiliation | Role |
|---|---|---|
| Adam Turpcu, PhD | Adverum Biotechnologies, Inc. | Study Director |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Adverum Clinical Site 223 | Gilbert | Arizona | 85297 | United States | ||
| Adverum Clinical Site 178 |
Adverum is committed to transparency.
Appropriately de-identified participant-level data and supporting documents may be shared under appropriate conditions (e.g. when contractually permitted and when participants provide appropriate consent). Individual patient-level data would only be shared following completion of this study (and any associated studies), completion of applicable regulatory submissions, and in accordance with applicable regulations and laws, as well as criteria established by Adverum, our collaborators and/or industry best practices. Shared datasets and/or documents may be de-identified and/or redacted to protect the identity of participants and to protect sensitive and confidential information.
For inquiries, please contact us at datasharing@adverum.com.
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| Aflibercept |
| Drug |
Aflibercept will be administered intravitreally. |
|
| Percentage of participants with improved BCVA from Baseline through Week 56 and Week 104 | BCVA measured by ETDRS | Baseline through Week 56 and Week 104 |
| Mean change from Baseline in BCVA through Week 104 | BCVA measured by ETDRS | Baseline through Week 104 |
| Mean change from Week 1 in BCVA based on an average at Weeks 52 and 56 and at Week 104 | BCVA measured by ETDRS | Week 1 to Week 56 and Week 104 |
| Percentage of participants with BCVA of 73 letters or more from Week 4 through Week 56 and Week 104 | Week 4 through Week 56 and Week 104 |
| Mean change in Central Subfield Thickness (CST) from Baseline to Week 56 and Week 104 | CST as measured by spectral domain optical coherence tomography (SD-OCT) | Baseline to Week 56 and Week 104 |
| Percentage of participants with CST ≤ 300 μm at Week 56 and Week 104 | CST will be assessed by a CRC using SD-OCT | Week 56 and Week 104 |
| Mean number of CST fluctuations > 50 μm from Week 1 through Week 56 and Week 104 | CST will be assessed by a CRC using SD-OCT images and the mean number of fluctuations with thickness of more than 50 μm will be summarized | Week 1 through Week 56 and Week 104 |
| Percentage of participants with CST fluctuations > 50 μm from Week 1 through Week 56 and Week 104 | CST will be assessed using SD-OCT | Week 1 through Week 56 and Week 104 |
| Mean number of aflibercept IVT injections received from Week 4 through Week 104 | Week 4 through Week 104 |
| Percent reduction in mean rate of annualized anti-Vascular Endothelial Growth Factor (VEGF) injections after 56 weeks and 104 weeks of study treatment. | Percent reduction in mean rate of annualized anti-VEGF injections will be assessed (after 56 weeks and after 104 weeks of study treatment) relative to the reduction in mean rate of annualized anti-VEGF injections received in the year prior to screening in treatment-experienced participants | Week 56 and Week 104 |
| Percentage of participants who were aflibercept injection-free | Week 4 through Week 56 and through Week 104 |
| Percentage of participants who received 0 or 1 aflibercept injection | Week 4 through Week 56 and through Week 104 |
| Percentage of participants who receive 0, 1, or 2 aflibercept injections from Week 4 through Week 56 and through Week 104 | Week 4 through Week 56 and through Week 104 |
| Mean change in area of Choroidal Neovascularization (CNV) lesion from Baseline through Week 104 | CNV is the infiltration of abnormal blood vessels in the retina from the underlying choroid layer. It will be assessed by a CRC using SD-OCT. | Baseline through Week 104 |
| Mean change in macular volume from Baseline through Week 104 | Macular volume will be measured as part of the full ophthalmic examination. | Baseline through Week 104 |
| Percentage of participants without Intraretinal Fluid (IRF) through Week 104 | IRF will be assessed using SD-OCT | Through Week 104 |
| Percentage of participants without Subretinal Fluid (SRF) through Week 104 | SRF will be assessed using SD-OCT | Through Week 104 |
| Percentage of participants with dry retina (defined as no IRF or SRF) through Week 104 | Dry Retina will be assessed using SD-OCT | Through Week 104 |
| Time to dry retina | Dry retina is defined as no IRF or SRF (i.e., absence of both) and will be assessed using SD-OCT | Through Week 104 |
| Time to sustained dry retina | Sustained dry retina is defined as no IRF or SRF (i.e., absence of both) maintained for 2 consecutive visits. | Through Week 104 |
| Number of participants who experienced ocular adverse events | The number of participants who experience an ocular adverse event will be summarized. | Through Week 56 and Week 104 |
| Number of participants who experienced mild, moderate or severe ocular adverse events | The number of participants who experience a mild, moderate or severe ocular adverse event will be summarized. | Through Week 56 and Week 104 |
| Number of participants who experienced non-ocular adverse events | The number of participants who experience a non-ocular adverse event will be summarized. | Through Week 56 and Week 104 |
| Number of participants who experienced mild, moderate or severe non-ocular adverse events | The number of participants who experience a mild, moderate or severe non-ocular adverse event will be summarized. | Through Week 56 and Week 104 |
| Mean change in 25-item National Eye Institute Visual Function Questionnaire (NEI VFQ-25) total and subscale scores | The NEI VFQ-25 measures vision-targeted patient-reported outcomes of individuals with chronic eye diseases. It comprises 25 questions. The assessment generates an overall composite score and includes the following subscales: global vision rating, difficulty with near vision activities, difficulty with distance vision activities, limitations in social functioning due to vision, role limitations due to vision, dependency on others due to vision, mental health symptoms due to vision, driving difficulties, limitations with peripheral and color vision, and ocular pain. A decrease in the NEI VFQ-25 score represents an improvement in disease severity. | Day 1 to Week 28, Week 56, and Week 104 |
| Phoenix |
| Arizona |
| 85021 |
| United States |
| Adverum Clinical Site 126 | Phoenix | Arizona | 85053 | United States |
| Adverum Clinical Site 229 | Scottsdale | Arizona | 85255 | United States |
| Adverum Clinical Site 159 | Tucson | Arizona | 85704 | United States |
| Adverum Clinical Site 198 | Springdale | Arkansas | 72764 | United States |
| Adverum Clinical Site 109 | Bakersfield | California | 93309 | United States |
| Adverum Clinical Site 100 | Beverly Hills | California | 90211 | United States |
| Adverum Clinical Site 201 | Campbell | California | 95008 | United States |
| Adverum Clinical Site 172 | Encino | California | 91436 | United States |
| Adverum Clinical Site 169 | Fullerton | California | 92835 | United States |
| Adverum Clinical Site 224 | Huntington Beach | California | 92647 | United States |
| Adverum Clinical Site 215 | Redlands | California | 92374 | United States |
| Adverum Clinical Site 164 | Riverside | California | 92505 | United States |
| Adverum Clinical Site 140 | Sacramento | California | 95825 | United States |
| Adverum Clinical Site 212 | Sacramento | California | 95841 | United States |
| Adverum Clinical Site 175 | Santa Barbara | California | 93103 | United States |
| Adverum Clinical Site 202 | Torrance | California | 90503 | United States |
| Adverum Clinical Site 189 | Walnut Creek | California | 94598 | United States |
| Adverum Clinical Site 200 | Denver | Colorado | 80222 | United States |
| Adverum Clinical Site 116 | Lakewood | Colorado | 80228 | United States |
| Adverum Clinical Site 165 | Waterford | Connecticut | 06385 | United States |
| Adverum Clinical Site 184 | Deerfield Beach | Florida | 33064 | United States |
| Adverum Clinical Site 176 | Fort Lauderdale | Florida | 33308 | United States |
| Adverum Clinical Site 221 | Fort Myers | Florida | 33912 | United States |
| Adverum Clinical Site 168 | Jacksonville | Florida | 32216 | United States |
| Adverum Clinical Site 214 | Lakeland | Florida | 33805 | United States |
| Adverum Clinical Site 213 | Orlando | Florida | 32806 | United States |
| Adverum Clinical Site 230 | Pensacola | Florida | 32503 | United States |
| Adverum Clinical Site 124 | Pompano Beach | Florida | 33064 | United States |
| Adverum Clinical Site 183 | South Miami | Florida | 33143 | United States |
| Adverum Clinical Site 120 | St. Petersburg | Florida | 33711 | United States |
| Adverum Clinical Site 193 | Tampa | Florida | 33617 | United States |
| Adverum Clinical Site 182 | Augusta | Georgia | 30909 | United States |
| Adverum Clinical Site 179 | Oak Forest | Illinois | 60452 | United States |
| Adverum Clinical Site 207 | Oak Park | Illinois | 60304 | United States |
| Adverum Clinical Site 195 | Carmel | Indiana | 46032 | United States |
| Adverum Clinical Site 205 | Carmel | Indiana | 46032 | United States |
| Adverum Clinical Site 197 | Hagerstown | Maryland | 21740 | United States |
| Adverum Clinical Site 204 | Hagerstown | Maryland | 21740 | United States |
| Adverum Clinical Site 167 | Detroit | Michigan | 48201 | United States |
| Adverum Clinical Site 216 | Madison | Mississippi | 39110 | United States |
| Adverum Clinical Site 163 | Southaven | Mississippi | 38671 | United States |
| Adverum Clinical Site 190 | St Louis | Missouri | 63128 | United States |
| Adverum Clinical Site 171 | Teaneck | New Jersey | 07666 | United States |
| Adverum Clinical Site 225 | Liverpool | New York | 13088 | United States |
| Adverum Clinical Site 196 | Asheville | North Carolina | 28803 | United States |
| Adverum Clinical Site 234 | Cary | North Carolina | 27511 | United States |
| Adverum Clinical Site 186 | Durham | North Carolina | 27705 | United States |
| Adverum Clinical Site 211 | Greensboro | North Carolina | 27401 | United States |
| Adverum Clinical Site 220 | Hickory | North Carolina | 28602 | United States |
| Adverum Clinical Site 209 | Wake Forest | North Carolina | 27587 | United States |
| Adverum Clinical Site 219 | Winston-Salem | North Carolina | 27103 | United States |
| Adverum Clinical Site 181 | Erie | Pennsylvania | 16507 | United States |
| Adverum Clinical Site 110 | Philadelphia | Pennsylvania | 19107 | United States |
| Adverum Clinical Site 208 | Charleston | South Carolina | 29414 | United States |
| Adverum Clinical Site 222 | Ladson | South Carolina | 29456 | United States |
| Adverum Clinical Site 122 | West Columbia | South Carolina | 29169 | United States |
| Adverum Clinical Site 144 | Rapid City | South Dakota | 57701 | United States |
| Adverum Clinical Site 123 | Abilene | Texas | 79606 | United States |
| Adverum Clinical Site 127 | Austin | Texas | 78705 | United States |
| Adverum Clinical Site 108 | Bellaire | Texas | 77401 | United States |
| Adverum Clinical Site 227 | Burleson | Texas | 76028 | United States |
| Adverum Clinical Site 194 | Dallas | Texas | 75231 | United States |
| Adverum Clinical Site 188 | Houston | Texas | 77030 | United States |
| Adverum Clinical Site 218 | Katy | Texas | 77494 | United States |
| Adverum Clinical Site 162 | McAllen | Texas | 78503 | United States |
| Adverum Clinical Site 185 | San Antonio | Texas | 78240 | United States |
| Adverum Clinical Site 232 | San Marcos | Texas | 78666 | United States |
| Adverum Clinical Site 228 | Schertz | Texas | 78154 | United States |
| Adverum Clinical Site 107 | The Woodlands | Texas | 77384 | United States |
| Adverum Clinical Site 231 | The Woodlands | Texas | 77384 | United States |
| Adverum Clinical Site 199 | Lynchburg | Virginia | 24502 | United States |
| Adverum Clinical Site 131 | Spokane | Washington | 99204 | United States |
| Adverum Clinical Site 187 | Wausau | Wisconsin | 54403 | United States |
| ID | Term |
|---|---|
| D005128 | Eye Diseases |
| D001766 | Blindness |
| ID | Term |
|---|---|
| D014786 | Vision Disorders |
| D012678 | Sensation Disorders |
| D009461 | Neurologic Manifestations |
| D009422 | Nervous System Diseases |
| D012816 | Signs and Symptoms |
| D013568 | Pathological Conditions, Signs and Symptoms |
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| ID | Term |
|---|---|
| C533178 | aflibercept |
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