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    The Curious Case of Copper: Copper’s Novel Stress Response and its Effect on Combined Stress

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    Author
    Hull, Bradford T.
    Issue Date
    2025
    Keywords
    Aging
    C. elegans
    combined stress
    Copper
    novel stress
    Advisor
    Sutphin, George
    
    Metadata
    Show full item record
    Publisher
    The University of Arizona.
    Rights
    Copyright © is held by the author. Digital access to this material is made possible by the University Libraries, University of Arizona. Further transmission, reproduction, presentation (such as public display or performance) of protected items is prohibited except with permission of the author.
    Abstract
    Cells encounter various forms of stress over time–oxidative stress, protein misfolding, DNA damage–and respond by activating specific, well-defined stress response pathways. As we age, the burden of stress increases while our cells’ ability to deal with the resulting damage becomes diminished due to dysregulation of cellular stress response pathways. Copper is a well-studied physiological stressor that is implicated in a variety of age-associated diseases such as cancer, cardiovascular disease, and many more. Though generally considered to be an oxidative stressor, here I describe a novel stress response where copper creates toxicity through an alternate mechanism in C. elegans. I show that this toxicity is independent of the oxidative stress response and several other canonical stress response pathways and is dependent on several genes previously unassociated with copper stress. Next, I describe copper’s protective mechanisms over several other physiological stressors and show that, similar to the individual stress response, this protective mechanism is independent of the oxidative stress response. I select the CuSO4- NaCl combination for further investigation and begin to characterize the genes involved in the C. elegans transcriptional response to the combined stress, identifying several key genes with functions related to immune response, protein processing, and membrane carbohydrate binding activity. In addition to the copper work, I also develop a protocol for longitudinal monitoring of individual worm lifespan, healthspan, and fluorescence in an environment that mimics manual agar lifespan assays. Finally, I propose a set of guidelines for the C. elegans stress response field in order to set standards for experiments and make future work more directly comparable.
    Type
    text
    Electronic Dissertation
    Degree Name
    Ph.D.
    Degree Level
    doctoral
    Degree Program
    Graduate College
    Molecular & Cellular Biology
    Degree Grantor
    University of Arizona
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