论文信息 - Biological response to a synthetic cornea.

Biological response to a synthetic cornea.

We have designed a synthetic cornea that has a transparent hydrogel optic and a porous skirt. The device has been implanted in rabbit corneas. We have shown that keratocytes migrate into the device and deposit a complex extracellular matrix. The immediate response is detected in the surrounding stroma, and the secondary response is seen after cells have deposited a matrix in the disc. After implantation, a decrease in keratan sulfate accompanied by an increase in dermatan sulfate was detected in the surrounding tissue compared to the unwounded corneal stroma. The glycosaminoglycans in the disc resemble that of an injured stroma. The appearance of heparan sulfate and growth factors, bFGF and TGFbeta, was not detected until 6 weeks after implantation. The growth factors were detected at the interface between the device and the tissue and become more diffuse over time. Methods of controlled release in vivo were used to enhance the rate of fibroplasia and wound repair. While these were successful in the cornea itself, when combined with the synthetic cornea the response was magnified and the initial attempts yielded neovascularization and edema. Currently, efforts are being directed at controlling the release within the porous haptic so that fibroplasia is enhanced while minimizing an inflammatory response.

V. Trinkaus-Randall | M. Nugent | M A Nugent | V Trinkaus-Randall

[1] H. Leibowitz,et al. Quantitation of inflammation in the cornea. , 1974, A M A Archives of Ophthalmology.

[2] R. Banwatt,et al. In vivo fibroplasia of a porous polymer in the cornea. , 1991, Investigative ophthalmology & visual science.

[3] R. Banwatt,et al. Synthesis of stromal glycosaminoglycans in response to injury , 1995, Journal of cellular biochemistry.

[4] V Trinkaus-Randall,et al. Advances in polyvinyl alcohol hydrogel keratoprostheses: protection against ultraviolet light and fabrication by a molding process. , 1997, Journal of biomedical materials research.

[5] C. Kublin,et al. Quantitative analysis of collagen from normal developing corneas and corneal scars. , 1981, Current eye research.

[6] V. Trinkaus-Randall,et al. Progress in the development of a synthetic cornea , 1994, Progress in Retinal and Eye Research.

[7] E. Edelman,et al. Controlled Release of Fibroblast Growth Factor: Activity in Cell Culture , 1991 .

[8] M. Nugent,et al. Basic Fibroblast Growth Factor Binds Its Receptors, Is Internalized, and Stimulates DNA Synthesis in Balb/c3T3 Cells in the Absence of Heparan Sulfate* , 1996, The Journal of Biological Chemistry.

[9] R. Banwatt,et al. Effect of pretreating porous webs on stromal fibroplasia in vivo. , 1994, Journal of biomedical materials research.