DESCRIPTION (Investigator's Abstract): Near-ultraviolet light from
sunlight is known to increase the risk of formation of human cortical
cataracts. The mechanism of action of different wavelengths of near-UV
radiation on the lens is unknown at present. The focus of this study is to
quantitate the biological effectiveness of specific wavelengths of
radiation between 297 and 400 nm on the lens and lens constituents. Action
spectra for lens opacification by monochromatic wavelengths in UVB
(297-320nm) and UVA (320-400 nm) will be determined under biologically
meaningful conditions. Intact bovine and human lenses and homogenates will
be used. Spectroscopic techniques and protein crosslinking will be used to
assess the damage. Quantitative studies on the generation of specific
reactive oxygen species will be done, to assess their role in photodamage
at different wavelengths. Less than ten percent of UVB and 60 percent of
UVA reaches the human lens epithelium in vivo. However, UVB and not UVA
increased the risk of cortical cataract formation in a recent human
epidemiological study. The biological effects of UVB and UVA radiation on
lens epithelial cells are unknown at present. Quantitative action spectrum
studies on the cell survival, synthesis of newly synthesized proteins and
DNA damage in lens epithelial cells are planned in this study. These data
will provide quantitative information on the biological effects of near-UV
wavelengths on the epithelium. Normal human lenses of different ages
(infant, young and old), and cataractous lens epithelia will be
investigated to determine the mechanism of action of near-UV radiation of
the human lens in vivo. The long-term objective of this proposal is to
define a molecular mechanism for the changes in lens constituents and
obtain a better understanding of the link between photodamage and human
cataract formation.
No Sub Projects information available for 2R01EY005681-14
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