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Effects of endogenous PPAR agonist nitro-oleic acid on metabolic syndrome in obese Zucker rats

机译:内源性PPAR激动剂硝基油酸对肥胖Zucker大鼠代谢综合征的影响

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Nitroalkene derivatives of nitro-oleic acid (OA- NO_2) are endogenous lipid products with novel signaling properties, particularly the activation of PPARs. The goal of this proposal was to examine the therapeutic potential of this OA- NO_2 in treatment of obesity and obesity-related conditions in obese Zucker rats. The animals were randomly divided to receive OA- NO_2, oleic acid (OA), both at 7.5 g /kg/d, or vehicle ethanol via osmotic mini-pumps for 2 weeks. Following OA- NO_2 treatment, food intake was decreased as early as the first day and this effect appeared to persist throughout the experimental period. At day 14, body weight gain was significantly reduced by OA- NO_2 treatment. This treatment significantly reduced plasma triglyceride and almost normalized plasma free fatty acid and significantly increased plasma high-density lipid (HDL). The plasma TBARS and proteinuria were paralelly decreased. In contrast, none of these parameters were affected by OA treatment. After 14 days of OA- NO _2 treatment, hematocrit, a surrogate of fluid retention associated with PPAR agonists, remained unchanged. Together, these data demonstrated that OA- NO_2 may offer an effective and safe therapeutic intervention for obesity and obesity-related conditions.
机译:硝基油酸的硝基烯烃衍生物(OA-NO_2)是内源性脂质产物,具有新颖的信号传导特性,尤其是PPAR的激活。该提议的目的是检验该OA-NO_2在肥胖Zucker大鼠中的肥胖和肥胖相关病症的治疗潜力。通过渗透微型泵将动物随机分为两组,分别接受7.5 g / kg / d的OA-NO_2,油酸(OA)或赋形剂乙醇,共2周。 OA-NO_2处理后,最早在第一天就减少了食物摄入,并且这种效果在整个实验期间似乎一直存在。在第14天,通过OA-NO_2治疗,体重增加显着降低。该治疗显着降低血浆甘油三酸酯和几乎标准化的血浆游离脂肪酸,并显着提高血浆高密度脂质(HDL)。血浆TBARS和蛋白尿平行降低。相反,这些参数均不受OA处理的影响。 OA-NO _2处理14天后,血细胞比容(与PPAR激动剂相关的体液滞留的替代物)保持不变。总之,这些数据表明,OA-NO_2可能为肥胖症和肥胖相关疾病提供有效且安全的治疗干预。

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