The major long-term objective of this program is a better understanding of the precataractous changes in elemental composition which occur at the cellular level in highly localized regions of the lens. This includes localized changes in the electrolytes, Na, K, and Cl, which may precede the onset of hydration and opacification. An understanding of how such changes are related to the development of cataracts, and how this information may be useful in development of procedures to prevent or delay the onset of cataractogenesis is the long term goal. The application of energy dispersive x-ray analysis in conjunction with scanning electron microscopy to the quantitative elemental analysis of individual cells and groups of cells in the normal and cataractous lens is the primary methodology for achieving these goals. The diffusible elements, notably Na, K, and Cl, will be studied in rapidly-frozen lens tissue. Cryosections containing superficial fibers, epithelium, and capsule in their normal structural relationship as well as other regions of the normal and cataractous lens, will be used along with internal standards. Also, lenses which have been rapidly-frozen along with internal standards, fractured and dried, will provide bulk specimens for elemental profiles of the whole lens, or for small defined regions of the normal or cataractous lens identified by CCRG photography. The major effort will be directed toward quantitative elemental analysis in lenses at various stages leading up to and including the early stages of opacification in the rat galactose cataract, the Nakano mouse cataract and the ouabain-induced cataract in the cultured rabbit lens, and at various stages during the reversal of the galactose cataract. Human cataracts, particularly supranuclear, will be analyzed for the concentrations of electrolytes in the opacities as compared to the transparent regions.

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY001874-11
Application #
3256276
Study Section
Visual Sciences A Study Section (VISA)
Project Start
1977-02-01
Project End
1990-01-31
Budget Start
1987-02-01
Budget End
1988-01-31
Support Year
11
Fiscal Year
1987
Total Cost
Indirect Cost
Name
Wayne State University
Department
Type
Schools of Medicine
DUNS #
City
Detroit
State
MI
Country
United States
Zip Code
48202
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Niyogi, T K; Emanuel, K; Parafina, J et al. (1991) The effects of iris-ciliary complex on the organ cultured rabbit ocular lens. Lens Eye Toxic Res 8:43-60
Banerjee, A; Richiert, D M; Emanuel, K et al. (1991) Studies on the possible role of vitreous humor on protein synthesis and morphology of organ cultured adult rabbit lens. II. Epithelial cells. Biochim Biophys Acta 1076:330-6
Bagchi, M; Emanuel, K (1991) Effect of vitreous humor on the organ cultured rabbit ocular lens. III. Morphology and elemental analysis. Lens Eye Toxic Res 8:449-67
Bagchi, M; Emanuel, K (1991) Elemental profiles in Emory mouse lens. Lens Eye Toxic Res 8:61-74
Banerjee, A; Richiert, D M; Bagchi, M (1991) Phosphorylation of small molecular weight polypeptides in the iris-ciliary complex, aqueous humor and vitreous humor. Biochim Biophys Acta 1077:56-64
Singh, A K; Bagchi, M (1989) Studies on the possible role of vitreous humor on the protein synthesis and clarity of the organ cultured ocular lens. Lens Eye Toxic Res 6:823-31
Harding, C V; Unakar, N J; Bagchi, M et al. (1989) Elemental and structural studies of the rat galactose cataract. Lens Eye Toxic Res 6:477-501
Lo, W K; Harding, C V (1986) Structure and distribution of gap junctions in lens epithelium and fiber cells. Cell Tissue Res 244:253-63