Pan-VEGF Blockade for the Treatment of Retinopathy of Prematurity

Part of paid clinical trials in Los Angeles, California.

Sponsor
Vision Research Foundation
Study ID
NCT00702819
Phase
PHASE1
Status
Terminated

Conditions

  • Retinopathy of Prematurity

Eligibility Criteria

Sex
ALL
Age
30 Weeks - 36 Weeks
Healthy Volunteers
Not accepted

Interventions

  • Bevacizumab — DRUG
    Dosage of 0.75mg/0.03ml injectable, one time only.

Study Details

Retinopathy of Prematurity (ROP) is a leading cause of blindness in children in developed countries around the world, and an increasing cause of blindness in developing countries. The retina lines the inside of the eye. It functions as "film" within the camera which is the eye. When an infant is born prematurely, the vascular network necessary to nourish the retina has not fully developed. As a consequence, in some infants abnormal vessels proliferate instead of the normal ones - a condition known as ROP. The abnormal vessels carry scar tissue along with them, and may lead to retinal detachment and blindness if the eye is not treated. The Multicenter Trial of Cryotherapy for Retinopathy of Prematurity (CRYO-ROP) Study demonstrated that ablation of the peripheral avascular retina reduced the risk of poor structural and visual outcome due to retinal distortion or detachment in ROP (1980's). The ablated retina is not functional and is not amenable to regeneration. Peripheral retinal ablation is not universally effective in fostering regression of ROP. This is particularly true for an aggressive form of ROP (aggressive posterior ROP, or APROP) which typically afflicts profoundly premature and infirm neonates. In this subset of infants, progression of ROP to bilateral retinal detachment and blindness occurs despite timely and complete peripheral retinal laser ablation. Rationale The development of ROP is largely dependent on vascular endothelial growth factor (VEGF). When an infant is born prematurely the relatively hyperoxic environment the baby is introduced to shuts down the production of VEGF. Retinal maturation is delayed. Subsequently, at a time when intraocular VEGF levels would normally be declining late in the third trimester of pregnancy, abnormally high levels of VEGF are seen due to large areas of avascular retina and associated tissue hypoxia. The availability of FDA-approved drugs for anti-VEGF treatment renders it possible to treat such eyes off-label. Available drugs include pegaptanib sodium (Macugen) for partial blockage of VEGF-A, or drugs such as ranibizumab (Lucentis) and bevacizumab (Avastin), which cause complete blockage of VEGF-A. As VEGF is required in the developing retina for normal angiogenesis, and our goal is not to penetrate tissue, but to block the excessive levels of VEGF trapped within the overlying vitreous which is responsible for the abnormal vasculature in ROP. For purposes of this study the investigators have chosen bevacizumab (Avastin), which will: a) attain complete blockage (vs. Macugen) of intravitreal VEGF-A, and; b) which is limited in its ability to penetrate tissues because it is a full antibody (vs. Lucentis, an antibody fragment specifically designed for better tissue penetration), and is more likely to restore VEGF homeostasis within the developing retina.

Key Dates

First listed
Jun 20, 2008
Start date
Jun 30, 2008
Status verified
Jun 2008
Primary completion
Jun 30, 2009
Completion
Jul 31, 2009

Study Design

Enrollment
2 participants (actual)
Allocation
NA
Intervention model
SINGLE_GROUP
Primary purpose
TREATMENT

Primary Outcome Measure

The primary aim is to evaluate the safety of Bevacizumab (Avastin) administered in a single dose into the vitreous cavity. [ Time Frame: Weekly ]

Locations (10)

FacilityCityStateZIPSite coordinators
Childrens HospitalLos AngelesCalifornia90027-
Jules Stein Eye CenterLos AngelesCalifornia90095-
California Vitreoretinal CenterMenlo ParkCalifornia94025-
Bascom Palmer Eye InstituteMiamiFlorida33136-
Emory Eye CenterAtlantaGeorgia30322-
Children's Hospital / Dept. OphthalmologyBostonMassachusetts02115-
William Beaumont HospitalRoyal OakMichigan48073-
University of North Carolina/OphthalmologyChapel HillNorth Carolina27599-7040-
University of Pennsylvania/Scheie Eye InstitutePhiladelphiaPennsylvania19104-
Baylor College of MedicineHoustonTexas77030-

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