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The need for a large-scale trial of fibrate therapy in diabetes: the rationale and design of the Fenofibrate Intervention and Event Lowering in Diabetes (FIELD) study. [ISRCTN64783481] |
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| Authors: | Iris J Edwards Janice D Wagner Catherine A Vogl-Willis Kenneth N Litwak William T Cefalu |
| Affiliation: | 1. Department of Pathology, Section on Comparative Medicine, Wake Forest University School of Medicine Winston-Salem, North Carolina, 27157-1047, USA 2. Department of Surgery-Thoracic, Cardiovascular Cardiovascular Research Center University of Louisville School of Medicine, 500 S. Floyd St Louisville, Kentucky, 40292, USA 3. Pennington Biomedical Research Center Louisiana State University, 6400 Perkins Road Baton Rouge, Louisiana, 70808, USA |
| Abstract: | BackgroundArterial proteoglycans are implicated in the pathogenesis of atherosclerosis by their ability to trap plasma lipoproteins in the arterial wall and by their influence on cellular migration, adhesion and proliferation. In addition, data have suggested an anti-atherogenic role for heparan sulfate proteoglycans and a pro-atherogenic role for dermatan sulfate proteoglycans. Using a non-human primate model for human diabetes, studies examined diabetes-induced changes in arterial proteoglycans that may increase susceptibility to atherosclerosis.MethodsControl (n = 7) and streptozotocin-induced diabetic (n = 8) cynomolgous monkeys were assessed for hyperglycemia by measurement of plasma glycated hemoglobin (GHb). Thoracic aortas obtained at necropsy, were extracted with 4 M guanidine HCL and proteoglycans were measured as hexuronic acid. Atherosclerosis was measured by enzymatic analysis of extracted tissue cholesterol. Glycosaminoglycan chains of arterial proteoglycans were released with papain, separated by agarose electrophoresis and analysed by scanning densitometry.ResultsTissue cholesterol was positively associated with hexuronic acid content in diabetic arteries (r = .82, p < .025) but not in control arteries. Glycosaminoglycan chain analysis demonstrated that dermatan sulfate was associated with increased tissue cholesterol in both control (r = .8, p < 0.05) and diabetic (r = .8, p < .025) arteries, whereas a negative relationship was observed between heparan sulfate and tissue cholesterol in diabetic arteries only (r = -.7, p < .05). GHb, which was significantly higher in diabetic animals (8.2 ± 0.9 vs 3.8 ± 0.2%, p < .0005) was negatively associated with heparan sulfate in diabetic arteries (r = -.7, p < .05).ConclusionsThese data implicate hyperglycemia induced modifications in arterial proteoglycans that may promote atherosclerosis. |
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