Abstract

Polyunsaturated fats can readily undergo peroxidation to yield lipid hydroperoxides that are potentially toxic to the intestine and other tissues when absorbed from the lumen. Despite previous attempts to study hydroperoxide absorption and its lymphatic transport, the factors that influence these processes are not known, and the metabolic fate of peroxidized lipids in the intestine remains poorly understood. An important aspect that has not been established is the role of glutathione (GSH) in the metabolism of lipid peroxides by the small intestine. Since GSH plays a key role in GSH peroxidase-catalyzed reduction of lipid peroxides, the status of mucosal GSH could significantly alter the metabolic fate of dietary peroxidized lipids. Therefore, the overall objective of this proposal is to characterize the effect of GSH on intestinal handling of luminal lipid hydroperoxides. We hypothesize that alterations in mucosal GSH will markedly affect the metabolism of lipid hydroperoxides at the level of absorption, mucosal degradation, lymphatic transport, and subsequent association with lipoproteins of lymph. To test this hypothesis, we propose the following specific aims: (1) To determine the effect of GSH deficiency on intestinal absorption and lymphatic transport of lipid hydroperoxides. (2) To investigate what effects exogenous GSH supplementation has on these processes. (3) To quantify the products derived from mucosal hydroperoxide metabolism. (4) To characterize and quantify associations of hydroperoxides with specific lipoprotein fractions of lymph. (5) To define the effects of fatty acid composition and fat content on hydroperoxide absorption and transport.
These aims will address three important aspects of intestinal handling of luminal peroxidized lipids: (a) the physiological significance of mucosal and exogenous GSH in hydroperoxide absorption and transport (Aims 1 & 2), (b) the function of GSH in intracellular processing of absorbed hydroperoxides (Aims 3 & 4), and (c) the influence of the type and quantity of luminal fat on hydroperoxide absorption and transport (Aim 5). For the proposed studies, the conscious, lymph fistula rat will be used. This model will allow us to quantify recoveries of lipid hydroperoxides in intestinal lumen, mucosa and lymph under steady-state conditions. The results of these studies will greatly enhance our understanding of the metabolism of dietary lipid hydroperoxides by the small intestine, and of the contributions of GSH and luminal fat to this process. The results should also provide useful information regarding the potential therapeutic benefits of dietary supplementation of GSH.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
1R01DK044510-01
Application #
3246035
Study Section
Nutrition Study Section (NTN)
Project Start
1992-02-01
Project End
1995-01-31
Budget Start
1992-02-01
Budget End
1993-01-31
Support Year
1
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Louisiana State University Hsc Shreveport
Department
Type
Schools of Medicine
DUNS #
City
Shreveport
State
LA
Country
United States
Zip Code
71103

  Publications

Circu, Magdalena L; Maloney, Ronald E; Aw, Tak Yee (2017) Low glucose stress decreases cellular NADH and mitochondrial ATP in colonic epithelial cancer cells: Influence of mitochondrial substrates. Chem Biol Interact 264:16-24
Wang, Bin; Aw, Tak Yee; Stokes, Karen Y (2016) The protection conferred against ischemia-reperfusion injury in the diabetic brain by N-acetylcysteine is associated with decreased dicarbonyl stress. Free Radic Biol Med 96:89-98
Li, Wei; Maloney, Ronald E; Aw, Tak Yee (2015) High glucose, glucose fluctuation and carbonyl stress enhance brain microvascular endothelial barrier dysfunction: Implications for diabetic cerebral microvasculature. Redox Biol 5:80-90
Busu, C; Atanasiu, V; Caldito, G et al. (2014) Influence of GSH synthesis inhibition on temporal distribution of NAD+/NADH during vascular endothelial cells proliferation. J Med Life 7:611-8
Xia, Hui; Mathew, Bobby; John, Tom et al. (2013) Microfluidic based immunosensor for detection and purification of carbonylated proteins. Biomed Microdevices 15:519-30
Bu?u, Carmina; Li, Wei; Caldito, Gloria et al. (2013) Inhibition of glutathione synthesis in brain endothelial cells lengthens S-phase transit time in the cell cycle: Implications for proliferation in recovery from oxidative stress and endothelial cell damage. Redox Biol 1:131-139
Li, Wei; Maloney, Ronald E; Circu, Magdalena L et al. (2013) Acute carbonyl stress induces occludin glycation and brain microvascular endothelial barrier dysfunction: role for glutathione-dependent metabolism of methylglyoxal. Free Radic Biol Med 54:51-61
Circu, Magdalena L; Aw, Tak Yee (2012) Intestinal redox biology and oxidative stress. Semin Cell Dev Biol 23:729-37
Xia, Hui; Murray, Kermit; Soper, Steven et al. (2012) Ultra sensitive affinity chromatography on avidin-functionalized PMMA microchip for low abundant post-translational modified protein enrichment. Biomed Microdevices 14:67-81
Circu, Magdalena L; Aw, Tak Yee (2012) Glutathione and modulation of cell apoptosis. Biochim Biophys Acta 1823:1767-77

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