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    Lipid profilling of polyunsaturated fatty acid - treated mouse brain and plasma. Investigation into polyunsaturated fatty acid (PUFA)-induced neuroprotection

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    ANEST WILLIAMS PHD THESIS WITH CORRECTIONS.pdf (11.45Mb)
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    Publication date
    2010-08-19T14:56:25Z
    Author
    Williams, Anest
    Supervisor
    Obrenovitch, Tihomir P.
    Nicolaou, Anna
    Keyword
    Mouse
    ; Fatty acids
    ; Brain
    ; Cortex
    ; Phospholipid
    ; Plasma
    ; Tandem mass spectrometry
    ; Neuroprotection
    ; Alpha linolenic acid; ALA
    ; Lipidomic analysis
    Rights
    Creative Commons License
    The University of Bradford theses are licenced under a Creative Commons Licence.
    Institution
    University of Bradford
    Department
    School of Pharmacy
    Awarded
    2010
    
    Metadata
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    Abstract
    Pre-treatment with polyunsaturated fatty acids or bioactive lipid mediators has been shown to reduce neuronal injury in rodent models of focal ischaemia, but the molecular mechanisms underlying this neuroprotection are unclear. In this study, we aimed to investigate whether systemic administration of alpha linolenic acid (ALA) leads to changes in the profile of mouse brain phospholipid and bioactive lipid mediators in both mouse brain and plasma within the previously determined neuroprotection time window. Mass spectrometry (MS) and tandem mass spectrometry (MS/MS) allowed us to detect and identify 47 phospholipids in mouse cerebral cortex, including several phospholipid species not previously reported in brain lipidomic studies. These included a phosphatidylethanolamine species with m/z 720 that has been associated with retinal stem cells. No widespread changes in cerebral cortex phospholipid composition were observed following intravenous ALA. Several significant changes in lipid mediators (P<0.05 with two-way ANOVA and post hoc Dunnett¿s t test) were detected in ALA-treated animals compared to untreated and vehicle-injected animals. Many of the affected lipid mediators are ligands for prostanoid receptors which have been demonstrated to play a role in the development of brain injury following cerebral ischaemia, implying that changes in bioactive lipid mediators or modulation of prostanoid receptors may occur following ALA pre-treatment in mice. This study illustrates the potential of advanced lipidomic analysis as a novel tool for neurochemists.
    URI
    http://hdl.handle.net/10454/4414
    Type
    Thesis
    Qualification name
    PhD
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