Li_2013_J.Lipid.Res_54_1608

Reference

Title : Ambient ultrafine particles alter lipid metabolism and HDL anti-oxidant capacity in LDLR-null mice - Li_2013_J.Lipid.Res_54_1608
Author(s) : Li R , Navab M , Pakbin P , Ning Z , Navab K , Hough G , Morgan TE , Finch CE , Araujo JA , Fogelman AM , Sioutas C , Hsiai T
Ref : J Lipid Res , 54 :1608 , 2013
Abstract :

Exposure to ambient particulate matter (PM) is a risk factor for cardiovascular diseases. The redox-active ultrafine particles (UFPs) promote vascular oxidative stress and inflammatory responses. We hypothesized that UFPs modulated lipid metabolism and anti-oxidant capacity of high density lipoprotein (HDL) with an implication in atherosclerotic lesion size. Fat-fed low density lipoprotein receptor-null (LDLR(-)/(-) mice were exposed to filtered air (FA) or UFPs for 10 weeks with or without administering an apolipoprotein A-I mimetic peptide made of D-amino acids, D-4F. LDLR(-)/(-) mice exposed to UFPs developed a reduced plasma HDL level (P < 0.01), paraoxonase activity (P < 0.01), and HDL anti-oxidant capacity (P < 0.05); but increased LDL oxidation, free oxidized fatty acids, triglycerides, serum amyloid A (P < 0.05), and tumor necrosis factor alpha (P < 0.05), accompanied by a 62% increase in the atherosclerotic lesion ratio of the en face aortic staining and a 220% increase in the cross-sectional lesion area of the aortic sinus (P < 0.001). D-4F administration significantly attenuated these changes. UFP exposure promoted pro-atherogenic lipid metabolism and reduced HDL anti-oxidant capacity in fat-fed LDLR(-)/(-) mice, associated with a greater atherosclerotic lesion size compared with FA-exposed animals. D-4F attenuated UFP-mediated pro-atherogenic effects, suggesting the role of lipid oxidation underlying UFP-mediated atherosclerosis.

PubMedSearch : Li_2013_J.Lipid.Res_54_1608
PubMedID: 23564731

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Citations formats

Li R, Navab M, Pakbin P, Ning Z, Navab K, Hough G, Morgan TE, Finch CE, Araujo JA, Fogelman AM, Sioutas C, Hsiai T (2013)
Ambient ultrafine particles alter lipid metabolism and HDL anti-oxidant capacity in LDLR-null mice
J Lipid Res 54 :1608

Li R, Navab M, Pakbin P, Ning Z, Navab K, Hough G, Morgan TE, Finch CE, Araujo JA, Fogelman AM, Sioutas C, Hsiai T (2013)
J Lipid Res 54 :1608