Inhibition of Migration for PVR Treatment
Motility, Inc., San Diego CA
Investigators
Abstract
DESCRIPTION (provided by applicant): Proliferative vitreoretinopathy (PVR) is the principal cause of failed retinal detachment surgery. PVR is characterized by the migration and proliferation of retinal pigment cells, fibroblasts, glial cells, and inflammatory cells on or beneath the retina or in the vitreous cavity. This leads to the formation of contractile cellular membranes which cause retinal detachment. Attempts to treat PVR have involved the use of antimetabolites and steroids. None of these options have come into routine clinical use and current interventions are limited to surgical treatment. While inhibition of cell proliferation has been the focus of the development of drugs to treat PVR, the possibility that cell migration, which plays as important of a role, would be another potential target. We have developed a small molecular weight protein (LD22-4) that inhibits the migration of a number of different cell types in vitro and in vivo. Because of the importance of cell migration in the development of PVR and the proven effectiveness of LD22-4 in vivo, we performed pilot studies of the effect of the protein in a rabbit model of PVR. The results clearly showed that LD22-4 inhibited the development of PVR in each animal that received the protein. Based on these considerations, we propose a more extensive evaluation of the effects of LD22-4 on PVR. The Phase I project will include two Specific Aims: 1. Dose titration analysis to establish effective doses for maximum inhibition of PVR 2. Time course study to determine the minimum number of injections needed to inhibit PVR. These results will provide the basis for the eventual use of LD22-4 in the treatment of PVR.
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