Abstract

The broad, long term objectives of this study are to (I) identify and characterize the growth factor-receptor systems through which the functions of corneal, immune, and other cells of the anterior segment of the eye are controlled during development, homeostasis, and wound healing; (II) understand at the molecular and cellular level, the factors that lead to corneal opacity, and its resolution, after injury, surgery or infecion; (III) explore the mechanism of epithelial basement membrane (EBM) regeneration after injury, including the role of corneal stromal cells in EBM regeneration, and the importance of the corneal EBM in modulating epithelial-stromal interactions in the cornea, including the development of myofibroblasts associated with stromal opacity. Photorefractive keratectomy (PRK) and irregular phototherapeutic keratectomy (PTK) are reproducible models of corneal stromal opacity that occurs after surgery, injury or infection.
The Specific aims of this proposal are to test the hypotheses that 1) the full structural regeneration of the corneal EBM, including the lamina lucida and lamina densa, a) occurs over a period of several days after injury to the epithelium, EBM and stroma, b) depends on the contribution of critical EBM components from stromal cells, in addition to epithelial cells; 2) in corneas that develop stromal opacity after hih correction PRK, the epithelial basement membrane does not regenerate properly because myofibroblasts that are generated after injury do not produce, or correctly localize, basement membrane components required for EBM regeneration and persist as a barrier to block keratocyte/ corneal fibroblast contributions of critical components needed for EBM regeneration; 3) that cultured keratocytes, corneal fibroblasts and myofibroblasts (keratocyte-derived and bone marrow-derived) have differential expression of EBM components that contribute to the lamina lucida and lamina densa of the EBM; and 4) that a) bone marrow-derived cell precursors to myofibroblasts in the cornea are fibrocytes, b) that the proportion of myofibroblasts in a cornea with haze derived from bone marrow-derived precursors compared to myofibroblasts derived from keratocyte-derived precursors increases in proportion to the extent of stromal injury and c) regeneration of EBM entails cytokine- mediated epithelial-stromal interactions mediated by interleukin-1 that regulate the expression of EBM components by keratocytes.

Public Health Relevance

The health relatedness of this project is that it is likely to provide a better understanding of 1) the regeneration of the corneal epithelial basement membrane after surgery, injury, or infection and 2) the pathogenesis and treatment of corneal stromal scaring that occurs with corneal surgery, injury, infections such as herpes simplex keratitis or disease. The research design is histopathological, cellular, and molecular investigations in corneas and cultured cells from animal models.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY010056-24
Application #
9692007
Study Section
Diseases and Pathophysiology of the Visual System Study Section (DPVS)
Program Officer
Mckie, George Ann
Project Start
1994-08-01
Project End
2021-04-30
Budget Start
2019-05-01
Budget End
2020-04-30
Support Year
24
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Cleveland Clinic Lerner
Department
Other Basic Sciences
Type
Schools of Medicine
DUNS #
135781701
City
Cleveland
State
OH
Country
United States
Zip Code
44195

  Publications

Medeiros, Carla S; Marino, Gustavo K; Lassance, Luciana et al. (2018) The Impact of Photorefractive Keratectomy and Mitomycin C on Corneal Nerves and Their Regeneration. J Refract Surg 34:790-798
Lassance, Luciana; Marino, Gustavo K; Medeiros, Carla S et al. (2018) Fibrocyte migration, differentiation and apoptosis during the corneal wound healing response to injury. Exp Eye Res 170:177-187
Wilson, Steven E; Medeiros, Carla S; Santhiago, Marcony R (2018) Pathophysiology of Corneal Scarring in Persistent Epithelial Defects After PRK and Other Corneal Injuries. J Refract Surg 34:59-64
Medeiros, Carla S; Marino, Gustavo K; Santhiago, Marcony R et al. (2018) The Corneal Basement Membranes and Stromal Fibrosis. Invest Ophthalmol Vis Sci 59:4044-4053
Medeiros, Carla S; Lassance, Luciana; Saikia, Paramananda et al. (2018) Posterior stromal cell apoptosis triggered by mechanical endothelial injury and basement membrane component nidogen-1 production in the cornea. Exp Eye Res 172:30-35
Saikia, Paramananda; Thangavadivel, Shanmugapriya; Medeiros, Carla S et al. (2018) IL-1 and TGF-? Modulation of Epithelial Basement Membrane Components Perlecan and Nidogen Production by Corneal Stromal Cells. Invest Ophthalmol Vis Sci 59:5589-5598
Saikia, Paramananda; Medeiros, Carla S; Thangavadivel, Shanmugapriya et al. (2018) Basement membranes in the cornea and other organs that commonly develop fibrosis. Cell Tissue Res 374:439-453
Santhanam, Abirami; Marino, Gustavo K; Torricelli, Andre A M et al. (2017) EBM regeneration and changes in EBM component mRNA expression in stromal cells after corneal injury. Mol Vis 23:39-51
Marino, Gustavo K; Santhiago, Marcony R; Santhanam, Abirami et al. (2017) Epithelial basement membrane injury and regeneration modulates corneal fibrosis after pseudomonas corneal ulcers in rabbits. Exp Eye Res 161:101-105
Wilson, Steven E; Marino, Gustavo K; Torricelli, Andre A M et al. (2017) Injury and defective regeneration of the epithelial basement membrane in corneal fibrosis: A paradigm for fibrosis in other organs? Matrix Biol 64:17-26

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