Treatment of Advanced Dry Age Related Macular Degeneration With AAVCAGsCD59
| Status: | Active, not recruiting |
|---|---|
| Conditions: | Ocular |
| Therapuetic Areas: | Ophthalmology |
| Healthy: | No |
| Age Range: | 50 - Any |
| Updated: | 3/7/2019 |
| Start Date: | March 29, 2017 |
| End Date: | December 6, 2019 |
A Phase 1, Open-Label, Multi-Center, Dose-Escalating, Safety and Tolerability Study of a Single Intravitreal Injection of AAVCAGsCD59 in Patients With Advanced Non-Exudative (Dry) Age-Related Macular Degeneration With Geographic Atrophy
Age related macular degeneration (AMD) is the leading cause of vision loss in individuals
over age 60. AMD is classified as wet and dry. Wet AMD constitutes 10 to 15% of all cases of
AMD and occurs when an abnormal blood vessel grows in or under the retina leading to central
vision loss. Wet AMD is successfully treated with injections in the eye on a monthly basis
that stop the blood vessel from growing and leaking. The most common form of AMD is the dry
variant or dry AMD that affects 85 to 90% of all patients with AMD. In dry AMD, there is loss
of retinal pigment, formation of deposits called drusen, and loss of the vessels in a layer
of the retina called the choriocapillaris. In the most severe forms of dry AMD there is loss
of retinal tissue called geographic atrophy. Over time retinal tissue degenerates in the area
responsible for central vision leading to vision loss leading to legal blindness. Currently
no treatment for dry AMD exists so that there is a significant unmet need in patients with
this ocular disease.
Recently, evidence has implicated an overactive inflammatory cascade called the complement
system as playing a pivotal role in the development of dry AMD. The complement cascade
consists of 3 arms that converge to form a pore-like complex on the surface of cells called
the membrane attack complex (MAC). Accumulation of MAC on cell surfaces leads to cell damage
and death causing the clinical findings seen in AMD. Normal cells within the human body
produce a protein on their cell surfaces called CD59 that blocks the MAC from forming. In
AMD, the complement cascade is upregulated and leads to more MAC formation than the body can
protect itself against leading to cell destruction.
AAVCAGsCD59, an ocular gene therapy product that is injected in to the eye in the physician's
office, causes normal retinal cells to increase the expression of a soluble form of CD59
(sCD59). This soluble recombinant version of the naturally occurring CD59 is designed and
intended to protect retinal cells that are responsible for central vision by inhibiting the
formation of the membrane attack complex (MAC), the terminal step of complement-mediated cell
lysis. In gene therapy the cells of the retina are potentially permanently altered to make
sCD59 for the life of the patient. With gene therapy only one injection is needed for the
drug to be effective for the patient's entire life. This study will evaluate the safety after
a single injection of AAVCAGsCD59 administered in an office setting for patients whose
enrolled eye has advanced dry AMD with geographic atrophy. The initial study is 26 weeks
followed by an additional 18-month safety evaluation.
over age 60. AMD is classified as wet and dry. Wet AMD constitutes 10 to 15% of all cases of
AMD and occurs when an abnormal blood vessel grows in or under the retina leading to central
vision loss. Wet AMD is successfully treated with injections in the eye on a monthly basis
that stop the blood vessel from growing and leaking. The most common form of AMD is the dry
variant or dry AMD that affects 85 to 90% of all patients with AMD. In dry AMD, there is loss
of retinal pigment, formation of deposits called drusen, and loss of the vessels in a layer
of the retina called the choriocapillaris. In the most severe forms of dry AMD there is loss
of retinal tissue called geographic atrophy. Over time retinal tissue degenerates in the area
responsible for central vision leading to vision loss leading to legal blindness. Currently
no treatment for dry AMD exists so that there is a significant unmet need in patients with
this ocular disease.
Recently, evidence has implicated an overactive inflammatory cascade called the complement
system as playing a pivotal role in the development of dry AMD. The complement cascade
consists of 3 arms that converge to form a pore-like complex on the surface of cells called
the membrane attack complex (MAC). Accumulation of MAC on cell surfaces leads to cell damage
and death causing the clinical findings seen in AMD. Normal cells within the human body
produce a protein on their cell surfaces called CD59 that blocks the MAC from forming. In
AMD, the complement cascade is upregulated and leads to more MAC formation than the body can
protect itself against leading to cell destruction.
AAVCAGsCD59, an ocular gene therapy product that is injected in to the eye in the physician's
office, causes normal retinal cells to increase the expression of a soluble form of CD59
(sCD59). This soluble recombinant version of the naturally occurring CD59 is designed and
intended to protect retinal cells that are responsible for central vision by inhibiting the
formation of the membrane attack complex (MAC), the terminal step of complement-mediated cell
lysis. In gene therapy the cells of the retina are potentially permanently altered to make
sCD59 for the life of the patient. With gene therapy only one injection is needed for the
drug to be effective for the patient's entire life. This study will evaluate the safety after
a single injection of AAVCAGsCD59 administered in an office setting for patients whose
enrolled eye has advanced dry AMD with geographic atrophy. The initial study is 26 weeks
followed by an additional 18-month safety evaluation.
Inclusion Criteria:
- Men or women 50 years of age or older
- Advanced dry AMD with GA in the study eye
- BCVA Snellen equivalent of 20/80 or worse in the study eye using ETDRS charts at a
starting distance of 4m after the first 3 patients are enrolled and demonstrate
favorable safety data
- Total GA lesion size 5mm2 (2 DA) to 20mm2 (8 DA) in the study eye; if multifocal, then
at least one focus of GA needs to measure 1.27 mm2 (0.5 DA)
- Fellow eye BCVA of 20/800 or better and must be the eye with the better visual acuity
- Must be willing to undergo paracentesis of the anterior chamber
Exclusion Criteria:
- GA secondary to non AMD etiologies
- Prior or active choroidal neovascularization (CNV) in the study eye
- History of conditions in the study eye during screening which might alter visual
acuity or interfere with study testing
- Active uncontrolled glaucoma
- Intraocular surgery in the study eye within 3 months of enrollment or are known or
likely candidate for intraocular surgery (including cataract surgery) in the study eye
within 1 year of treatment
- Acute or chronic infection in the study eye
- History of inflammation in the study eye or ongoing inflammation in either eye
- History of uveitis in the study eye
- Ongoing ocular inflammation in either eye
- Any contraindication to intravitreal injection
- Currently using or have used treatment for exudative AMD in the study eye only: laser
photocoagulation, photodynamic therapy (PDT), ranibizumab (Lucentis®), pegaptanib
sodium (Macugen®), bevacizumab (Avastin®) or aflibercept (Eylea®)
- Currently using any periocular (study eye), intravitreal (study eye) or systemic (oral
or intravenous) corticosteroids within 3 months prior to screening.
- Any of the following underlying systemic diseases:
- Unstable or severe cardiovascular disease, e.g., congestive heart failure (New
York Heart Association Functional class III or IV), myocardial infarction within
6 months, ventricular tachyarrhythmias requiring ongoing treatment, unstable
angina, or critical limb ischemia;
- Poorly controlled diabetes;
- Clinically significant impaired renal or hepatic function, for example:
- Cerebrovascular disease within 12 months prior to Screening;
- Dementia or neurodegenerative disease (e.g., Alzheimer's disease, Parkinson's
disease);
- Have a malignancy at Screening or a history of malignancy that precludes
completion of this 2-year study, including presence of tumor or disease whose
treatment may directly affect the ability to evaluate the safety and efficacy of
AAVCAGsCD59, or currently undergoing treatment for a specific cancer;
- Immunocompromised conditions and/or need for immunosuppressive therapy;
- Any significant poorly controlled illness that would preclude study compliance and
follow-up
- Current or prior use of any medication known to be toxic to the retina or optic nerve
including, but not limited, to chloroquine/hydrochloroquine, deferoxamine,
phenothiazines and ethambutol
- Previous treatment with any ocular or systemic gene transfer product
- Received any investigational product within 120 days prior to screening
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