DESCRIPTION (Adapted from the investigator's Abstract): The main purpose of the
proposed studies is to test the validity of the oxidative stress hypothesis of
aging, which postulates that the age-associated loss of functional capacity is
substantially due to the accrual of molecular oxidative damage. The focus of
this study is to investigate one of the main predictions of this hypothesis,
namely that variations in the level of oxidative stress, induced by
experimental alterations in antioxidative defenses, should correspondingly
affect the rate of aging. Specifically, this study will determine the effects
of an increased or a decreased ability of cells to synthesize and regenerate
reduced glutathione (GSH) on the aging process of Drosophila melanogaster. GSH
can react with a variety of free radical species and, in conjunction with
superoxide dismutase, provide the main mechanism or the attenuation of
oxidative stress. Flies that have an increased ability to synthesize and
regenerate GSH will be created by the transgenic overexpression of
gamma-glutamylcysteine synthetase (the rate-limiting enzyme in GSH synthesis)
and glucose-6-phosphate dehydrogenase (which generates NADPH, required for
reduction of oxidized glutathione to GSH), respectively. In contrast, flies
with a decreased ability to synthesize and regenerate GSH will be obtained by
isolating mutant alleles of these genes. The effects of over-and
under-expression of these genes on life span and a variety of
biochemical/physiological alterations, related to the aging process, will be
determined. Subsequently, the effects of co-overexpression of these genes with
other antioxidative genes (e. Cu,Zn-superoxide dismutase and catalase) on the
aging process of the flies will be determined. Results should (i) provide a
direct test of the role of the genes, involved in the maintenance of GSH, in
the aging process, (ii) permit further assessment of the validity of the
oxidative stress hypothesis of aging, and (iii) aid in the design of similar
studies in mammals.
No Sub Projects information available for 2R01AG015122-04
Publications
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No Outcomes available for 2R01AG015122-04
Clinical Studies
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