Abstract

Neovascularization of the cornea is a significant cause of decreased visual acuity and blindness. It occurs in patients with trachoma and herpetic keratitis as well as in traumatic, inflammatory, toxic and nutritional disorders. The progression of corneal neovascularization in experimental animals involves many distinct phases which can be broadly divided into: 1) a prevascular latent period; 2) a stage of neovascularization; and 3) a stage of vascular regression. Potential angiogenic factors responsible for neovascularization include mediators and components of the inflammatory response such as leukocytes, platelets, fibrin, eicosanoids and plasminogen activator. Corneal vascularization is markedly suppressed by total body irradiation. This is presumed to be largely secondary to radiation induced leukopenia which impairs the leukocytic infiltration into the cornea and to a lesser extent due to the effect of irradiation of the pericorneal vascularization. To further investigate the association of corneal neovascularization and leukocytes, we will study the effect of syngeneic bone marrow transplantation on the reversibility of the suppression of corneal angiogenesis in inbred irradiated rats. Fischer 344 inbred rats will receive either total body irradiation, irradiation of the head alone, or irradiation of the body alone. Control rats will receive no irradiation. Some rats receiving total body irradiation will undergo syngeneic bone marrow transplantation immediately following irradiation. Six days after irradiation when the peripheral leukocytic counts reach their lowest level following total body irradiation, corneas will be cauterized with silver/potassium nitrate under standard conditions that are known to reproducibly induce corneal neovascularization in the rat. Four days after injury, rats will be sacrificed and the vasculature will be immediately perfused with gelatin containing colloidal carbon. Corneal flat preparations will be analyzed in a masked fashion to quantitate corneal vascularization objectively by measurement of the resultant carbon filled corneal blood vessels by a computerized image analysis. The effects of irradiation and bone marrow reconstitution will be assessed by sequential complete blood counts, flow cytometry analysis of lymphocyte and mononuclear subsets in the peripheral blood and bone marrow and histologic examination of eyes and bone marrows.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Physician Scientist Award (K11)
Project #
1K11EY000304-01A1
Application #
3086785
Study Section
Vision Research and Training Committee (VSN)
Project Start
1989-07-01
Project End
1994-12-31
Budget Start
1989-07-01
Budget End
1990-12-31
Support Year
1
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Duke University
Department
Type
Schools of Medicine
DUNS #
071723621
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Scroggs, M W; Proia, A D; Charles, N C et al. (1993) Calcific phacolysis. Ophthalmology 100:377-83
Scroggs, M W; Proia, A D (1992) Histopathological variation in keratoconus. Cornea 11:553-9
Scroggs, M W; Lewis, J S; Proia, A D (1992) Corneal argyrosis associated with silver soldering. Cornea 11:264-9
Scroggs, M W; Klintworth, G K (1991) Senile scleral plaques: a histopathologic study using energy-dispersive x-ray microanalysis. Hum Pathol 22:557-62
Scroggs, M W; Proia, A D; Smith, C F et al. (1991) The effect of total-body irradiation on corneal neovascularization in the Fischer 344 rat after chemical cauterization. Invest Ophthalmol Vis Sci 32:2105-11
Scroggs, M W; Johnston, W W; Klintworth, G K (1990) Intraocular tumors. A cytopathologic study. Acta Cytol 34:401-8
Scroggs, M W; Chandler, D B; Klintworth, G W (1990) Acid hematin pigmentation of the cornea in stillborn fetuses. Pediatr Pathol 10:319-33