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    Exposure to a Three-Phthalate Mixture Tampers with Lipid Metabolic Processes in the Ovarian Antral Follicle Microenvironment

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    Name:
    azu_etd_22140_sip1_m.pdf
    Embargo:
    2027-05-27
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    8.921Mb
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    Author
    Miller, Kara Leann
    Issue Date
    2025
    Keywords
    Infertility
    Lipid Metabolism
    Ovarian Follicle
    Ovary
    Phthalate
    Proteome
    Advisor
    Craig, Zelieann R.
    
    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.
    Embargo
    Release after 05/27/2027
    Abstract
    Phthalates are a family of endocrine disrupting chemicals with ubiquitous exposure in humans. Dibutyl phthalate (DBP), di-2-ethylhexylphthalte (DEHP), and benzyl butyl phthalate (BBP) are used in personal care, medical, and pharmaceutical products. Antral follicles within the ovary are essential for ovulation and downstream fertilization and pregnancy. DBP, BBP, and DEHP are known to associate with decreased antral follicle counts in women and inhibit mouse antral follicle growth and ovulation in vitro. However, the specific mechanism of toxicity driving these outcomes is largely unknown. Therefore, the aim of the studies outlined in this dissertation address this gap in knowledge by investigating the effects of a three-phthalate mixture on the antral follicle microenvironment. Proteome and lipidome profiling of antral follicles from CD-1 female mice exposed in-vivo to an environmentally relevant dose of a mixture of DBP, BBP, and DEHP revealed that lipid metabolic processes are targeted. Lipidomic analysis of serum and liver tissues from matched mice highly suggested that lipid changes are not occurring through a systemic mechanism. While in vitro treatment of DBP, BBP, DEHP on mouse primary granulosa cells highlighted the ability of this mixture of phthalates to modulate expression of enzymes through activation of peroxisome proliferator activated receptor gamma (PPAR). Overall, these studies demonstrate that phthalates target the antral follicle microenvironment resulting in increased saturated free fatty acid levels, reduced shuttling of carnitines for beta oxidation, and diminished triglyceride stores, which is likely occurring through activated intracellular PPAR and secondary signaling mechanisms.
    Type
    text
    Electronic Dissertation
    Degree Name
    Ph.D.
    Degree Level
    doctoral
    Degree Program
    Graduate College
    Pharmacology & Toxicology
    Degree Grantor
    University of Arizona
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